Electrophysiologic Testing

Electrophysiologic Testing FO U R TH E DITION Richard N. Fogoros, MD Pittsburgh, PA Electrophysiologic Testing For ...

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Electrophysiologic Testing FO U R TH E DITION

Richard N. Fogoros, MD Pittsburgh, PA

Electrophysiologic Testing

For Anne, Emily and Joe, who maintain my rhythms

Electrophysiologic Testing FO U R TH E DITION

Richard N. Fogoros, MD Pittsburgh, PA

© 2006 Richard N. Fogoros Published by Blackwell Publishing Ltd Blackwell Publishing, Inc., 350 Main Street, Malden, Massachusetts 02148-5020, USA Blackwell Publishing Ltd, 9600 Garsington Road, Oxford OX4 2DQ, UK Blackwell Publishing Asia Pty Ltd, 550 Swanston Street, Carlton, Victoria 3053, Australia The right of the Author to be identiﬁed as the Author of this Work has been asserted in accordance with the Copyright, Designs and Patents Act 1988. All rights reserved. No part of this publication may be reproduced, stored in a retrieval system, or transmitted, in any form or by any means, electronic, mechanical, photocopying, recording or otherwise, except as permitted by the UK Copyright, Designs and Patents Act 1988, without the prior permission of the publisher. First published 1990 (Blackwell Science, Inc.) Second edition 1994 (Blackwell Science, Inc.) Third edition 1999 (Blackwell Science, Inc.) Fourth edition 2006 Library of Congress Cataloging-in-Publication Data Fogoros, Richard N. Electrophysiologic testing / Richard N. Fogoros. – 4th ed. p. ; cm. Includes bibliographical references and index. ISBN-13: 978-1-4051-0478-4 (pbk. : alk. paper) ISBN-10: 1-4051-0478-3 (pbk. : alk. paper) 1. Arrhythmia–Diagnosis. 2. Invasive electrophysiologic testing. I. Title. [DNLM: 1. Arrhythmia–Diagnosis. 2. Arrhythmia–therapy. 3. Electrophysiology. WG 330 F656e 2006] RC685.A65F64 2006 616.1'2807547–dc22 2005034908 ISBN-13: 978-1-4051-04784 ISBN-10: 1-4051-04783 A catalogue record for this title is available from the British Library Set in 9.75 on 12 pt minion by SNP Best-set Typesetter Ltd., Hong Kong Printed and bound in India by Replika Press PVT Ltd. Acquisitions: Gina Almond Development Editor: Simone Dudziak Production Controller: Kate Charman For further information on Blackwell Publishing, visit our website: http://www.blackwellcardiology.com The publisher’s policy is to use permanent paper from mills that operate a sustainable forestry policy, and which has been manufactured from pulp processed using acidfree and elementary chlorine-free practices. Furthermore, the publisher ensures that the text paper and cover board used have met acceptable environmental accreditation standards. Notice: The indications and dosages of all the drugs in this book have been recommended in the medical literature and conform to the practices of the general community. The medications described do not necessarily have speciﬁc approval by the Food and Drug Administration for use in the diseases and dosages for which they are recommended. The package insert for each drug should be consulted for use and dosage as approved by the FDA. Because standards for usage change, it is advisable to keep abreast of revised recommendations, particularly those concerning new drugs

Contents

Preface to the Fourth Edition, vii Acknowledgements, viii Part I: Disorders of the Heart Rhythm: Basic Principles, 1

1 The Cardiac Electrical System, 3 2 Abnormal Heart Rhythms, 12 3 Treatment of Arrhythmias, 22 Part II: The Electrophysiology Study in the Evaluation and Therapy of Cardiac Arrhythmias, 33

4 Principles of the Electrophysiology Study, 35 5 The Electrophysiology Study in the Evaluation of the SA Node, AV Node and His-Purkinje System, 58 6 The Electrophysiology Study in the Evaluation of Supraventricular Tachyarrhythmias, 103 7 The Electrophysiology Study in the Evaluation and Treatment of Ventricular Arrhythmias, 158 8 Transcatheter Ablation: Therapeutic Electrophysiology, 211 9 Cardiac Resynchronization: Pacing Therapy for Heart Failure, 253 10 The Evaluation of Syncope, 266 11 Electrophysiologic Testing in Perspective: The Evaluation and Treatment of Cardiac Arrhythmias, 278 Index, 288

v

Preface to the Fourth Edition

It is gratifying to me that Electrophysiologic Testing has continued to generate an audience through three editions, and especially gratifying that that audience has remained the one I originally intended. When this book was ﬁrst written, there were no other books available that attempted to explain and de-mystify the arcane world of the electrophysiologist to students, residents, cardiology fellows, primary care physicians, cardiologists, nurses, and technicians. Now that there are a few others that do so, I am very pleased that readers continue to ﬁnd this one useful. I have made extensive revisions to this fourth edition. Chapters 5 and 7 have been completely rewritten, Chapters 6 and 8 have been substantially revised, Chapter 9 is entirely new, and smaller changes have been made throughout. Despite making these many changes, I have attempted diligently to adhere to my original intent — to provide a quick and relatively painless introduction to the ﬁeld of cardiac electrophysiology. This latest edition continues to emphasize the basic principles of electrophysiology, and to show how those principles underlie the testing (and the therapy) that take place in the electrophysiology laboratory, as well as the clinical decisions made by electrophysiologists, whether or not those decisions involve invasive testing. I would like to thank once again the many readers who took the time to let me know that this volume has made a difference in their professional lives. It is that, above everything else, which has motivated me to continue working hard to keep this project relevant and useful. Richard N. Fogoros, MD

vii

Acknowledgements

I would like to acknowledge the suggestions made to me by several readers as to how I could improve this book. I hope at least a few of you ﬁnd evidence herein that your advice was listened to. I would especially like to thank Liz Bush, Principal Systems Engineer at St Jude Medical, who suggested to me a few years ago (after listening to me lecture on matters electrophysiologic for a day and a half), that my book would be much better if only I would ﬁx numerous typos and other small errors. When I explained that I had ﬁxed all the errors I knew about, she rolled her eyes and said she would make a list. I had forgotten the exchange entirely until last year, when I was about to begin work on this present edition. Out of the blue I received an e-mail from Liz — her list was ready. It was a much longer list than I had thought possible, but every item on it accurately identiﬁed something that required my attention. Liz, I have tried diligently to ﬁx every problem you identiﬁed (and, if only to spare you any more work, have also tried diligently not to introduce any new ones). I deeply appreciate all the time you spent on this, and I am truly gratiﬁed that a busy professional such as yourself cared enough about this project to extend such an effort. Finally, I would like to thank my wife Anne and my children Emily and Joe, who, once again, lovingly accepted the periods of moodiness and inattentiveness that seem to accompany my working on new editions of Electrophysiologic Testing. Without their love and support, neither this book nor anything else I might have accomplished in life would seem the least bit worthwhile.

viii

PA R T I

Disorders of the Heart Rhythm: Basic Principles

CHAPTER 1

The Cardiac Electrical System

The heart spontaneously generates electrical impulses, and these electrical impulses are vital to all cardiac functions. On a basic level, by controlling the ﬂux of calcium ions across the cardiac cell membrane, these electrical impulses trigger cardiac muscle contraction. On a higher level, the heart’s electrical impulses organize the sequence of muscle contraction during each heartbeat, important for optimizing the cardiac stroke volume. Finally, the pattern and timing of these impulses determine the heart rhythm. Derangements in this rhythm often impair the heart’s ability to pump enough blood to meet the body’s demands. Thus, the heart’s electrical system is fundamental to cardiac function. The study of the electrical system of the heart is called cardiac electrophysiology, and the main concern of the ﬁeld of electrophysiology is with the mechanisms and therapy of cardiac arrhythmias. The electrophysiology study is the most deﬁnitive method of evaluating the cardiac electrical system; it is the subject of this book. As an introduction to the ﬁeld of electrophysiology and to the electrophysiology study, this chapter reviews the anatomy of the cardiac electrical system and describes how the vital electrical impulse is normally generated and propagated.

The anatomy of the heart’s electrical system The heart’s electrical impulse originates in the sinoatrial (SA) node, located high in the right atrium near the superior vena cava. The impulse leaves the SA node and spreads radially across both atria. When the impulse reaches the atrioventricular (AV) groove, it encounters the “skeleton of the heart,” the ﬁbrous structure to which the valve rings are attached, and that separates the atria from the ventricles. This ﬁbrous structure is electrically inert and acts as an insulator — the electrical 3

4

I Disorders of the Heart Rhythm: Basic Principles

impulse cannot cross this structure. Thus, the electrical impulse would be prevented from crossing over to the ventricular side of the AV groove if not for the specialized AV conducting tissues: the AV node and the bundle of His (Figure 1.1). As the electrical impulse enters the AV node, its conduction is slowed because of the electrophysiologic properties of the AV nodal tissue. This slowing is reﬂected in the PR interval on the surface electrocardiogram (ECG). Leaving the AV node, the electrical impulse enters the His bundle, the most proximal part of the rapidly conducting His-Purkinje system. The His bundle penetrates the ﬁbrous skeleton and delivers the impulse to the ventricular side of the AV groove. Once on the ventricular side, the electrical impulse follows the His bundle as it branches into the right and left bundle branches. Branching of the Purkinje ﬁbers continues distally to the furthermost reaches of the ventricular myocardium. The electrical impulse is thus rapidly distributed throughout the ventricles.

Fig. 1.1 Anatomy of the electrical system of the heart.

1 The Cardiac Electrical System

5

Hence, the heart’s electrical system is designed to organize the sequence of myocardial contraction with each heartbeat. As the electrical impulse spreads over the atria toward the AV groove, the atria contract. The delay provided by the AV node allows for complete atrial emptying before the electrical impulse reaches the ventricles. Once the impulse leaves the AV node, it is distributed rapidly throughout the ventricular muscle by the Purkinje ﬁbers, providing for brisk and orderly ventricular contraction. We next consider the character of the electrical impulse, its generation, and propagation.

The cardiac action potential The cardiac action potential is one of the most despised and misunderstood topics in cardiology. The fact that electrophysiologists claim to understand it is also a leading cause of the mystique that surrounds them and their favorite test, the electrophysiology study. Because the purpose of this book is to debunk the mystery of electrophysiology studies, we must confront the action potential and learn to understand it. Fortunately, this is far easier than legend would have it. Although most of us would like to think of cardiac arrhythmias as an irritation or “itch” of the heart (and of antiarrhythmic drugs as a balm or a salve that soothes the itch), this conceptualization of arrhythmias is wrong and leads to the faulty management of patients with arrhythmias. In fact, the behavior of the heart’s electrical impulse and of the cardiac rhythm is largely determined by the shape of the action potential; the effect of antiarrhythmic drugs is determined by how they change that shape. The inside of the cardiac cell, like all living cells, has a negative electrical charge compared to the outside of the cell. The resulting voltage difference across the cell membrane is called the transmembrane potential. The resting transmembrane potential (which is −80 to −90 mV in cardiac muscle) is the result of an accumulation of negatively charged molecules (called ions) within the cell. Most cells are happy with this arrangement and live out their lives without considering any other possibilities. Cardiac cells, however, are excitable cells. When excitable cells are stimulated appropriately, tiny pores or channels in the cell membrane open and close sequentially in a stereotyped fashion. The opening of these channels allows ions to travel back and forth across the cell membrane (again in a stereotyped fashion), leading to patterned changes in the transmembrane potential. When these stereotypic voltage changes are graphed against time, the result is the cardiac action

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I Disorders of the Heart Rhythm: Basic Principles

Fig. 1.2 The cardiac action potential.

potential (Figure 1.2). The action potential is thus a reﬂection of the electrical activity of a single cardiac cell. As can be seen in Figure 1.2, the action potential is classically divided into ﬁve phases. However, it is most helpful to consider the action potential in terms of three general phases: depolarization, repolarization, and the resting phase. Depolarization

The depolarization phase (phase 0) is where the action of the action potential is. Depolarization occurs when the rapid sodium channels in the cell membrane are stimulated to open. When this happens, positively charged sodium ions rush into the cell, causing a rapid, positively directed change in the transmembrane potential. The resultant voltage spike is called depolarization. When we speak of the heart’s electrical impulse, we are speaking of this depolarization. Depolarization of one cell tends to cause adjacent cardiac cells to depolarize, because the voltage spike of a cell’s depolarization causes the sodium channels in the nearby cells to open. Thus, once a cardiac cell is stimulated to depolarize, the wave of depolarization (the electrical impulse) is propagated across the heart, cell by cell. Further, the speed of depolarization of a cell (reﬂected by the slope of phase 0 of the action potential) determines how soon the next cell will

1 The Cardiac Electrical System

7

depolarize, and thus determines the speed at which the electrical impulse is propagated across the heart. If we do something to change the speed at which sodium ions enter the cell (and thus change the slope of phase 0), we therefore change the speed of conduction (the conduction velocity) of cardiac tissue. Repolarization

Once a cell is depolarized, it cannot be depolarized again until the ionic ﬂuxes that occur during depolarization are reversed. The process of getting the ions back to where they started is called repolarization. The repolarization of the cardiac cell roughly corresponds to phases 1 through 3 (i.e., the width) of the action potential. Because a second depolarization cannot take place until repolarization occurs, the time from the end of phase 0 to late in phase 3 is called the refractory period of cardiac tissue. Repolarization of the cardiac cells is complex and poorly understood. Fortunately, the main ideas behind repolarization are simple: 1) repolarization returns the cardiac action potential to the resting transmembrane potential; 2) it takes time to do this; 3) the time that it takes to do this, roughly corresponding to the width of the action potential, is the refractory period of cardiac tissue. There is an additional point of interest regarding repolarization of the cardiac action potential. Phase 2 of the action potential, the so-called plateau phase, can be viewed as interrupting and prolonging the repolarization that begins in phase 1. This plateau phase, which is unique to cardiac cells (e.g., it is not seen in nerve cells), gives duration to the cardiac potential. It is mediated by the slow calcium channels, which allow positively charged calcium ions to slowly enter the cell, thus interrupting repolarization and prolonging the refractory period. The calcium channels have other important effects in electrophysiology, as we will see. The resting phase

For most cardiac cells, the resting phase (the period of time between action potentials, corresponding to phase 4) is quiescent, and there is no net movement of ions across the cell membrane. For some cells, however, the so-called resting phase is not quiescent. In these cells, there is leakage of ions back and forth across the cell membrane during phase 4 in such a way as to cause a gradual increase in transmembrane potential (Figure 1.3). When the transmembrane potential is high enough (i.e., when it reaches the threshold voltage), the appropriate channels are activated to cause the cell to depolarize.

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I Disorders of the Heart Rhythm: Basic Principles

Fig. 1.3 Automaticity. In some cardiac cells, there is a leakage of ions across the cell membrane during phase 4 in such a way as to cause a gradual, positively directed change in transmembrane voltage. When the transmembrane voltage becomes sufﬁciently positive, the appropriate channels are activated to automatically generate another action potential. This spontaneous generation of action potentials due to phase 4 activity is called automaticity.

Because this depolarization, like any depolarization, can stimulate nearby cells to depolarize in turn, the spontaneously generated electrical impulse can be propagated across the heart. This phase 4 activity, which leads to spontaneous depolarization, is called automaticity. Automaticity is the mechanism by which the normal heart rhythm is generated. Cells in the SA node (the pacemaker of the heart) normally have the fastest phase 4 activity within the heart. The spontaneously occurring action potentials in the SA node are propagated as described earlier, resulting in normal sinus rhythm. If, for any reason, the automaticity of the sinus node should fail, there are usually secondary pacemaker cells (often located in the AV junction) that take over the pacemaker function of the heart, but at a slower rate. Thus, the shape of the action potential determines the conduction velocity, refractory period, and automaticity of cardiac tissue. Later we shall see how these three electrophysiologic characteristics directly affect the mechanisms of cardiac rhythms, both normal and abnormal. To a large extent, the purpose of the electrophysiology study is to assess the conduction velocities, refractory periods, and automaticity of various portions of the heart’s electrical system.

Localized variations in the heart’s electrical system In understanding cardiac arrhythmias, it is important to consider two issues involving localized differences in the heart’s electrical system: variations in the action potential and variations in autonomic innervation.

1 The Cardiac Electrical System

9

Localized differences in the action potential

The cardiac action potential does not have the same shape in every cell of the heart’s electrical system. The action potential we have been using as a model (see Figure 1.2) is a typical Purkinje ﬁber action potential. Figure 1.4 shows representative action potentials from several key locations of the heart — note the differences in shape. The action potentials that differ most radically from the Purkinje ﬁber model are found in the SA node and AV node. Note that the action potentials from these tissues have slow instead of rapid depolarization phases (phase 0). This slow depolarization occurs because SA nodal and AV nodal tissues lack the rapid sodium channels responsible for the rapid depolarization phase (phase 0) seen in other cardiac tissues. In fact, the SA and AV nodes are thought to be dependent entirely on the slow calcium channel for depolarization. Because the speed of depolarization determines conduction velocity, the SA and AV nodes conduct electrical impulses slowly. The slow conduction in the AV node is reﬂected in the PR interval on the surface ECG (see Figure 1.5). Localized differences in autonomic innervation

In general, an increase in sympathetic tone causes enhanced automaticity (pacemaker cells ﬁre more rapidly), increased conduction velocity (electrical impulses are propagated more rapidly), and decreased action potential duration and thus decreased refractory periods (cells are ready for repeated depolarizations more quickly). Parasympathetic tone has

Fig. 1.4 Localized differences in the cardiac action potential. Cardiac action potentials from different locations within the heart have different shapes. These differences account for the differences seen in electrophysiologic properties in various tissues within the heart.

10 I Disorders of the Heart Rhythm: Basic Principles

Fig. 1.5 Relationship between the ventricular action potential (top) and the surface ECG (bottom). The rapid depolarization phase (phase 0) of the action potential is reﬂected in the QRS complex on the surface ECG. Because phase 0 is almost instantaneous, the QRS complex yields directional information on ventricular depolarization. In contrast, the repolarization portion of the action potential has signiﬁcant duration (phases 2 and 3). Consequently, the portion of the surface ECG that reﬂects repolarization (the ST segment and the T wave) yields little directional information. PR interval, beginning of P to beginning of QRS; ST segment, end of QRS to beginning of T; QT interval, beginning of QRS to end of T.

the opposite effect (i.e., depressed automaticity, decreased conduction velocity, and increased refractory periods). Sympathetic and parasympathetic ﬁbers richly innervate both the SA node and the AV node. In the remainder of the heart’s electrical system, while sympathetic innervation is abundant, parasympathetic innervation is relatively sparse. Thus, changes in parasympathetic tone have a relatively greater effect on the SA nodal and AV nodal tissues than on other tissues of the heart. This fact has implications for the diagnosis and treatment of some heart rhythm disturbances.

1 The Cardiac Electrical System 11

Relationship between action potential and surface ECG The cardiac action potential represents the electrical activity of a single cardiac cell. The surface ECG reﬂects the electrical activity of the entire heart — essentially, it represents the sum of all the action potentials of all cardiac cells. Consequently, the information one can glean from the surface ECG derives from the characteristics of the action potential (Figure 1.5). For most cardiac cells, the depolarization phase of the action potential is essentially instantaneous (occurring in 1 to 3 msec) and occurs sequentially, from cell to cell. Thus, the instantaneous wave of depolarization can be followed across the heart by studying the ECG. The P wave represents the depolarization front as it traverses the atria, and the QRS complex tracks the wave of depolarization as it spreads across the ventricles. Changes in the spread of the electrical impulse, such as occur in bundle branch block or in transmural myocardial infarction, can be readily diagnosed. Because the depolarization phase of the action potential is relatively instantaneous, the P wave and the QRS complex can yield speciﬁc directional information (i.e., information on the sequence of depolarization of cardiac muscle). In contrast, the repolarization phase of the action potential is not instantaneous — indeed, repolarization has signiﬁcant duration. Thus, while depolarization occurs from cell to cell sequentially, repolarization occurs in many cardiac cells simultaneously. For this reason, the ST segment and T wave (the portions of the surface ECG that reﬂect ventricular repolarization) give little directional information, and abnormalities in the ST segments and T waves are most often (and quite properly) interpreted as being nonspeciﬁc. The QT interval represents the time of repolarization of the ventricular myocardium and reﬂects the average action potential duration of ventricular muscle.

CHAPTER 2

Abnormal Heart Rhythms

Abnormalities in the electrical system of the heart result in two general types of cardiac arrhythmias: heart rhythms that are too slow (bradyarrhythmias) and heart rhythms that are too fast (tachyarrhythmias). To understand the use of the electrophysiology study in evaluating cardiac arrhythmias, one needs a basic understanding of the mechanisms of these arrhythmias.

Bradyarrhythmias There are two broad categories of abnormally slow heart rhythms — the failure of pacemaker cells to generate appropriate electrical impulses (disorders of automaticity) and the failure to propagate electrical impulses appropriately (heart block). Failure of impulse generation

Failure of SA nodal automaticity, resulting in an insufﬁcient number of electrical impulses emanating from the SA node (i.e., sinus bradycardia [Figure 2.1]), is the most common cause of bradyarrhythmias. If the slowed heart rate is insufﬁcient to meet the body’s demands, symptoms result. Symptomatic sinus bradycardia is called sick sinus syndrome. If sinus slowing is profound, subsidiary pacemakers located near the AV junction can take over the pacemaker function of the heart. The electrophysiology study, as we will see in Chapter 5, can be useful in assessing SA nodal automaticity. Failure of impulse propagation

The second major cause of bradyarrhythmias is the failure of the electrical impulses generated by the SA node (or by subsidiary atrial pacemakers) to conduct normally to the ventricles. This condition, known as 12

2 Abnormal Heart Rhythms

13

Fig. 2.1 Sinus bradycardia.

heart block or AV block, implies an abnormality of conduction velocity and/or refractoriness in the conducting system. Because conduction of the electrical impulse to the ventricles depends on the function of the AV node and the His-Purkinje system, heart block is virtually always due to AV nodal or His-Purkinje disease. Heart block is classiﬁed into three categories based on severity (Figure 2.2). First-degree AV block means that, while all atrial impulses are transmitted to the ventricles, intraatrial conduction, conduction through the AV node, and/or conduction through the His bundle is slow (manifested on the ECG by a prolonged PR interval). Second-degree AV block means that conduction to the ventricles is intermittent; that is, some impulses are conducted and some are blocked. Third-degree AV block means that block is complete and no atrial impulses are conducted to the ventricles. If third-degree AV block is present, then sustaining life depends on the function of subsidiary pacemakers distal to the site of block. The competence of these subsidiary pacemakers, and therefore the patient’s prognosis, depends largely on the site of block (Figure 2.3). When block is within the AV node, subsidiary pacemakers at the AV junction usually take over the pacemaker function of the heart, resulting in a relatively stable, non–life-threatening heart rhythm, with a rate often in excess of 50 beats/min. On the other hand, if block is distal to the AV node, the subsidiary pacemakers tend to produce a profoundly slow (usually less than 40 beats/min) and unstable heart rhythm. If heart block is less than complete (i.e., ﬁrst- or second-degree), it is still important to pinpoint the site of block to either the AV node or the His-Purkinje system. First- or second-degree block in the AV node is benign and tends to be nonprogressive. Thus, implanting a permanent pacemaker is rarely required. First- and especially second-degree block distal to the AV node, on the other hand, tends to progress to a higher degree of block; prophylactic pacing is often indicated. Differentiating the site of heart block requires careful evaluation. This evaluation can usually be made noninvasively by studying the surface ECG and taking advantage of the AV node having rich autonomic innervation which the His-Purkinje system does not have. Sometimes,

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I Disorders of the Heart Rhythm: Basic Principles

Fig. 2.2 Three categories of heart block. In ﬁrst-degree block (top tracing), all atrial impulses are conducted to the ventricles, but conduction is slow (the PR interval is prolonged). In second-degree block (middle tracing), some atrial impulses are conducted and some are not. In third-degree block (bottom tracing), none of the atrial impulses are conducted to the ventricles.

Fig. 2.3 Examples of escape pacemakers. When block is localized to the AV node (top tracing), junctional escape pacemakers (JE) are usually stable enough to prevent hemodynamic collapse. When block is located in the distal conducting tissues (bottom tracing), escape pacemakers are usually located in the ventricles (VE) and are slower and much less stable.

however, the electrophysiology study is useful in locating the site of block. Chapter 5 considers this in detail.

Tachyarrhythmias Cardiac tachyarrhythmias can cause signiﬁcant mortality and morbidity. It is the ability of the electrophysiology study to address the

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15

evaluation and treatment of tachyarrhythmias that has brought this procedure into widespread use. We will discuss three mechanisms for tachyarrhythmias — automaticity, reentry, and triggered activity. Automaticity

Automaticity has been discussed as a normal pacemaker function of the heart. When abnormal acceleration of phase 4 activity occurs in some location of the heart, an automatic tachyarrhythmia is said to occur (Figure 2.4). Such an abnormal automatic focus can appear in the atria, the AV junction, or the ventricles (thus leading to automatic atrial, junctional, or ventricular tachycardia). Automaticity is not a common cause of tachyarrhythmias, probably accounting for less than 10% of all abnormal tachyarrhythmias. Automatic tachyarrhythmias are usually recognizable by their characteristics and the settings in which they occur. In gaining an understanding of the automatic tachyarrhythmias, it is helpful to consider the characteristics of sinus tachycardia, which is a normal automatic tachycardia. Sinus tachycardia usually occurs as a result of appropriately increased sympathetic tone (for instance, in response to increased metabolic needs during exercise). When sinus tachycardia develops, the heart rate gradually increases from the basic (resting) sinus rate; when sinus tachycardia subsides, the rate likewise decreases gradually. Similarly, automatic tachyarrhythmias often display a warm-up and warm-down in rate when the arrhythmia begins and ends. Analogous to sinus tachycardia, automatic tachyarrhythmias also often have metabolic causes, such as acute cardiac ischemia, hypoxemia, hypokalemia, hypomagnesemia, acid–base disorders, high sympathetic tone, and the use of sympathomimetic agents. Therefore, automatic arrhythmias are often seen in acutely ill patients, often in the intensive care setting, with all the attendant metabolic abnormalities. For example, acute pulmonary disease can lead to multifocal atrial tachycardia, the most common type of automatic atrial tachycardia. Induction of, and recovery from, general anesthesia can cause surges in sympathetic tone and automatic arrhythmias (both atrial and ventricular) can result. In addition, acute myocardial infarction is often accompanied by early ventricular arrhythmias which are most likely automatic in mechanism. Of all tachyarrhythmias, automatic arrhythmias resemble an “itch of the heart” the most closely, and it is tempting to apply the salve of antiarrhythmic drugs. Antiarrhythmic drugs can sometimes decrease automaticity; automatic arrhythmia, however, should be treated primarily by identifying and reversing the underlying metabolic cause.

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I Disorders of the Heart Rhythm: Basic Principles

Fig. 2.4 Abnormal automaticity causes the rapid generation of action potentials and thus inappropriate tachycardia.

Automatic tachyarrhythmias cannot be induced by programmed pacing techniques, so these arrhythmias are generally not amenable to provocative study in the electrophysiology laboratory. Reentry

Reentry is the most common mechanism for tachyarrhythmias; it is also the most important, because reentrant arrhythmias cause the deaths of hundreds of thousands of people every year. Fortunately, reentrant arrhythmias lend themselves nicely to study in the electrophysiology laboratory. It was the recognition that most tachyarrhythmias are reentrant in mechanism and that the electrophysiology study can help signiﬁcantly in assessing reentrant arrhythmias that led to widespread proliferation of electrophysiology laboratories since the early 1980s. Unfortunately, the mechanism of reentry is not simple to explain or to understand, and the prerequisites for reentry seem on the surface to be unlikely at best. The failure to understand (and possibly to believe in) reentry has helped keep the electrophysiology study an enigma to most people in the medical profession. The following explanation of reentry therefore errs on the side of simplicity and might offend some electrophysiologists. If the reader can keep an open mind and accept this explanation for now, we hope to show later (in Chapters 6 and 7) that reentry is a compelling explanation for most cardiac tachyarrhythmias. Reentry requires that the following criteria be met (Figure 2.5). First, two roughly parallel conducting pathways (shown as pathways A and B) must be connected proximally and distally by conducting tissue, thus forming a potential electrical circuit. Second, one of the pathways (pathway B in our example) must have a refractory period that is substantially longer than the refractory period of the other pathway. Third, the pathway with the shorter refractory period (pathway A) must conduct electrical impulses more slowly than the other pathway.

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Fig. 2.5 Prerequisites for reentry. An anatomic circuit must be present in which two portions of the circuit (pathways A and B in the ﬁgure) have electrophysiologic properties that differ from one another in a critical way. In this example, pathway A conducts electrical impulses more slowly than pathway B; pathway B has a longer refractory period than pathway A.

If all these seemingly implausible prerequisites are met, reentry can be initiated when an appropriately timed premature impulse is introduced to the circuit (Figure 2.6). The premature impulse must enter the circuit at a time when pathway B (the one with the long refractory period) is still refractory from the previous depolarization and at a time when pathway A (the one with the shorter refractory period) has already recovered and is able to accept the premature impulse. While pathway A slowly conducts the premature impulse, pathway B has a chance to recover. By the time the impulse reaches pathway B from the opposite direction, pathway B is no longer refractory and is able to conduct the beat in the retrograde direction (upward in the ﬁgure). If this retrograde impulse reenters pathway A and is conducted antegradely (as it is likely to do, given the short refractory period of pathway A), a continuously circulating impulse is established, spinning around and around the reentrant loop. All that remains in order for this reentrant impulse to usurp the rhythm of the heart is for the impulse to exit from the circuit at some point during each lap and thereby to depolarize the myocardium outside of the loop.

18 I Disorders of the Heart Rhythm: Basic Principles

Fig. 2.6 Initiation of reentry. If the prerequisites in Fig. 2.5 are present, then an appropriately timed premature impulse can block in pathway B (which has a relatively long refractory period) while conducting down pathway A. Because conduction down pathway A is slow, pathway B has time to recover, allowing the impulse to conduct retrogradely up pathway B. The impulse can then reenter pathway A. A continuously circulating impulse is thus established.

Just as reentry can be initiated by premature beats, it can be terminated by premature beats (Figure 2.7). An appropriately timed impulse can enter the circuit during reentry and collide with the reentrant impulse, thus abolishing the reentrant arrhythmia. Because reentry depends on critical differences in conduction velocities and refractory periods in the various pathways of the reentrant circuit, and because conduction velocity and refractory periods are determined by the shape of the action potential, it should be obvious that the action potentials in pathway A and pathway B are different from one another. This means furthermore that drugs that change the shape of the action potential might be useful in the treatment of reentrant arrhythmias. Reentrant circuits occur with some frequency in the human heart. Some reentrant circuits are present at birth, especially those causing supraventricular tachycardias (e.g., reentry associated with AV bypass

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19

Fig. 2.7 Termination of reentry. An appropriately timed premature impulse can enter the circuit during a reentrant tachycardia, collide with the reentrant impulse as shown, and terminate reentry.

tracts or with dual SA nodal and AV nodal tracts). More malignant forms of reentrant circuits, however, are usually not congenital but are acquired as cardiac disease develops during life. In reentrant ventricular tachyarrhythmias, the reentrant circuits arise in areas where normal cardiac tissue is interspersed with patches of scar tissue, forming many potential anatomic circuits. Thus, ventricular reentrant circuits usually occur only when scar tissue develops in the ventricles (such as during a myocardial infarction or with cardiomyopathic diseases). Theoretically, if all the anatomic and electrophysiologic criteria for reentry are present, any impulse that enters the circuit at the appropriate time will induce a reentrant tachycardia. The time from the end of the refractory period of pathway A to the end of the refractory period of pathway B, during which reentry can be induced, is called the tachycardia zone. Treating reentrant arrhythmias sometimes involves trying to narrow or abolish the tachycardia zone (by increasing the refractory period of pathway A or decreasing the refractory period of pathway B). Because reentrant arrhythmias can be reproducibly induced and terminated with appropriately timed impulses, reentrant arrhythmias are ideal for study in the electrophysiology laboratory. In fact, it is mainly

20

I Disorders of the Heart Rhythm: Basic Principles

the inducibility of reentrant arrhythmias that distinguishes them from automatic arrhythmias in the electrophysiology lab. By inducing reentrant arrhythmias in a controlled setting, the location of the anatomic circuit can be mapped and the effect of various therapies assessed. Triggered activity

Electrophysiologists try to divide the universe of tachyarrhythmias into two parts— automatic arrhythmias (which cannot be induced in the laboratory) and reentrant arrhythmias (which can be induced). This is a useful and practical way of thinking about tachyarrhythmias. Simple and convenient classiﬁcation systems are usually wrong, however, and this classiﬁcation system is no exception. There are other mechanisms for tachyarrhythmias, no doubt including some that have not yet been identiﬁed. While most of these other mechanisms can safely be ignored, at least one appears commonly in the clinical setting — triggered activity. Triggered activity has some features of both automaticity and reentry and can be difﬁcult to distinguish in the electrophysiology laboratory. Like automaticity, triggered activity involves the leakage of positive ions into the cardiac cell, leading to a bump on the action potential (Figure 2.8A) in late phase 3 or early phase 4. This bump is called an afterdepolarization. If these afterdepolarizations are of sufﬁcient magnitude to engage the rapid sodium channels (i.e., if they reach the threshold voltage), another action potential can be generated (Figure 2.8B). Thus, triggered activity resembles automaticity in that new action potentials can be generated by leakage of positive ions into the cell. Many electrophysiologists classify triggered activity as a subgroup of automaticity. Unlike automaticity (and like reentry), however, triggered activity is not always spontaneous (and therefore not truly automatic). Triggered activity can be provoked by premature beats. Thus, triggered activity, like reentry, can be induced with programmed pacing techniques. Theoretically, because it can be induced during electrophysiologic testing, triggered activity poses a potential threat to the use of the inducibility of an arrhythmia as the major criterion for diagnosing a reentrant mechanism. If an arrhythmia is induced, the following have been proposed as methods of differentiating between reentry and triggered automaticity: triggered activity resembles automaticity in displaying warm-up and warm-down; triggered activity is felt to depend on calcium channels and thus may respond to calcium channel blockers; in distinction to most reentrant arrhythmias, inducing arrhythmias due to triggered activity may require introducing a pause into the sequence of paced beats used for induction (such arrhythmias, called “pause-

2 Abnormal Heart Rhythms

21

Fig. 2.8 Triggered activity. (A) In some circumstances, premature cardiac action potentials will display a late bump (called an afterdepolarization). (B) If the afterdepolarization is of sufﬁcient magnitude, the rapid sodium channels are engaged and a second action potential is generated.

dependent” arrthythmias, will be discussed in Chapter 7); reentry is the more likely mechanism in the presence of underlying structural cardiac disease. The clinical signiﬁcance of triggered activity has become more clear over the past decade. Triggered activity is most likely the mechanism for digitalis-toxic supraventricular and ventricular arrhythmias, as well as for some of the rare cases of ventricular tachycardia that respond to calcium-blocking agents. More importantly, triggered activity is now thought to be the mechanism of torsades de pointes — the polymorphic, pause-dependent ventricular arrhythmias often associated with the use of certain antiarrhythmic drugs. Triggered activity as a cause of ventricular arrhythmias will be discussed more fully in Chapter 7.

CHAPTER 3

Treatment of Arrhythmias

Pharmacologic therapy Antiarrhythmic drugs are not arrhythmia suppressants in the same way that menthol is a cough suppressant. They do not work by soothing irritable areas. In fact, most antiarrhythmic drugs work merely by changing the shape of the cardiac action potential. By changing the action potential, these drugs alter the conductivity and refractoriness of cardiac tissue. Thus, it is hoped, the drugs will change the critical electrophysiologic characteristics of reentrant circuits to make reentry less likely to occur. Channels and gates

Antiarrhythmic drugs are thought to affect the shape of the action potential by altering the channels that control ionic ﬂuxes across the cardiac cell membrane. The class I antiarrhythmic drugs, which affect the rapid sodium channel, provide the clearest example (Figure 3.1). The rapid sodium channel is controlled by two gates: the m gate and the h gate. In the resting state (A), the m gate is closed and the h gate is open. When an appropriate stimulus occurs, the m gate opens (B) and positively charged sodium ions rush into the cell rapidly, causing the cell to depolarize (phase 0 of the action potential). After a few milliseconds, the h gate slams shut (C), closing the sodium channel and ending phase 0. Class I antiarrhythmic drugs work by binding to the h gate, making it behave as if it is partially closed (D). In this case, when the m gate is stimulated to open, the opening through which sodium ions enter the cell is narrower (E). Consequently, it takes longer to depolarize the cell (i.e., the slope of phase 0 is decreased). Because the speed of depolarization determines how quickly adjacent cells will depolarize (and therefore the 22

3 Treatment of Arrhythmias

23

Fig. 3.1 The effect of class I drugs on the rapid sodium channel. (A) through (C) display the baseline (drug-free) state. In (A), the resting state, the m gate is closed and the h gate is open. The cell is stimulated in (B), causing the m gate to open, thus allowing positively charged sodium ions to enter the cell rapidly (large arrow). In (C), the h gate shuts and sodium transport stops (i.e., phase 0 ends). (D) through (E) display the effect of adding a class I antiarrhythmic drug (open circles). (D) shows the class I drug binding to the h gate, making it behave as if it is partially closed. When the cell is stimulated in (E), the m gate still opens normally, but the channel through which sodium ions enter the cell is narrower and sodium transport is slower. It subsequently takes longer to reach the end of phase 0 (F), and the slope of phase 0 is decreased.

speed of impulse propagation), class I drugs as a group tend to decrease the conduction velocity of cardiac tissue. Although their precise sites of action have not all been worked out, most antiarrhythmic drugs act in a similar fashion, that is, by altering the function of the various channels that control transport of ions across cardiac cell membranes. The resultant changes in the cardiac action potential (Figure 3.2) cause changes in the conduction velocity, refractoriness, and automaticity of cardiac tissue, and also provide the basis for the classiﬁcation of antiarrhythmic drugs.

24

I Disorders of the Heart Rhythm: Basic Principles

Fig. 3.2 The effect of antiarrhythmic drugs on the cardiac action potential. The solid lines represent the baseline action potential and the dotted lines represent the changes that result in the action potential when various classes of antiarrhythmic drugs are given. The Purkinje ﬁber action potential is represented except in the case of class IV drugs, for which the AV nodal action potential is depicted.

Classiﬁcation of antiarrhythmic drugs

Table 3.1 lists the most frequently used classiﬁcation system for antiarrhythmic drugs. Class I is reserved for drugs that block the rapid sodium channel (as shown in Figure 3.1). Because drugs assigned to class I block the sodium channel in varying degrees and also have varying effects on action potential duration, class I is currently broken down into three subgroups (Table 3.2). Class Ia drugs (quinidine, procainamide, and disopyramide) slow conduction velocity and increase refractory periods. Class Ib drugs (lidocaine, tocainide, mexiletine, and phenytoin) actually have little effect on depolarization when used in systemic

3 Treatment of Arrhythmias

25

Table 3.1 Classiﬁcation of Antiarrhythmic Drugs. Class I

Bind to sodium channel, decrease speed of depolarization

Class II

β-blocking drugs, decrease sympathetic tone atenolol nadolol bisoprolol carvedilol labetolol propranolol metoprolol timolol Affect mainly SA and AV nodes (indirectly by blocking β receptors)

Class III

Increase action potential duration amiodarone N-acetylprocainamide bretylium sotalol ibutilide dofetilide

Class IV

Calcium channel blockers diltiazem verapamil Affect mainly SA and AV nodes (direct membrane effect, see Fig. 3.2)

Class V

Digitalis agents digitoxin digoxin Affect mainly SA and AV nodes (indirectly by increasing vagal tone)

Table 3.2 Subclassiﬁcation of Class I Antiarrhythmic Agents. Class Ia

Quinidine, procainamide, disopyramide slow upstroke of action potential + + prolong duration of action potential + + decrease conductivity, increase refractoriness

Class Ib

Lidocaine, phenytoin, tocainide, mexiletine minimal effect on upstroke of action potential shorten duration of action potential decrease refractoriness

Class Ic

Flecainide, encainide, propafenone, moricizine* marked slowing of upstroke of action potential + + + + minimal effect on action potential duration + marked decrease in conductivity, little effect on refractoriness

*The classiﬁcation of moricizine is controversial, and some place it in class Ib. It is placed in class Ic here to emphasize its class Ic–like proarrhythmic potential.

26

I Disorders of the Heart Rhythm: Basic Principles

doses (although in high concentrations these drugs, too, can block sodium transport — this is why lidocaine is an excellent local anesthetic agent). In systemic doses, class Ib drugs decrease action potential duration and shorten refractory periods but have little effect on conduction velocity. Class Ic drugs (ﬂecainide, encainide, and propafenone) have a pronounced depressant effect on conduction velocity, with relatively little effect on refractory periods. β-Blocking agents are assigned to class II. These drugs have little direct effect on the action potential and work mainly by decreasing the sympathetic tone. Class III drugs (amiodarone, bretylium, dofetilide, ibutilide, Nacetylprocainamide, and sotalol) increase the action potential duration and therefore refractory periods, and have relatively little effect on the conduction velocity. Class IV includes the calcium channel blockers. They mainly affect the SA and AV nodes, because these structures are almost exclusively depolarized by the slow calcium channels. Class V includes digitalis agents, whose antiarrhythmic effects are related to the increase in parasympathetic activity caused by these drugs. Effect of antiarrhythmic drugs

Most antiarrhythmic drugs are felt to ameliorate automatic tachyarrhythmias to some extent, although it must again be stressed that the primary treatment for automatic arrhythmias is to remove the underlying cause. Many antiarrhythmic drugs slow the phase 4 ionic ﬂuxes, which are responsible for automaticity. Figure 3.3 shows two examples of how antiarrhythmic drugs may affect reentrant circuits. Figure 3.3A shows a reentrant circuit with the same characteristics as described in Chapter 2. Figure 3.3B illustrates the changes that may occur if a class Ia drug is administered. These drugs increase refractory periods. By further lengthening the already long refractory period of pathway B, the class Ia drugs can convert unidirectional block to bidirectional block, thus chemically amputating one pathway of the reentrant circuit. Figure 3.3C shows what happens if a class Ib drug is given. These drugs shorten the duration of the action potential, thus decreasing the refractory period. In this example a class Ib drug shortens the refractory period of pathway B, thus rendering the refractory periods in pathway A and pathway B relatively equal. (In other words, the tachycardia zone is signiﬁcantly narrowed.) Without a difference in refractory periods between the two pathways of the anatomic circuit, reentry cannot be initiated.

3 Treatment of Arrhythmias

27

The drug effects illustrated in Figure 3.3 should not be taken literally. The key point in understanding how drugs affect reentry is this: because reentry requires a critical relationship between the refractory periods and the conduction velocities of the two pathways of the reentrant circuit, and because antiarrhythmic drugs alter the refractory periods and conduction velocities, these drugs can make reentry less likely to occur. Proarrhythmia

Unfortunately, there is another side to that coin. Consider the following scenario: A patient with a previous myocardial infarction and complex ventricular ectopy (but no sustained tachyarrhythmias) has an anatomic circuit whose electrophysiologic characteristics are like those shown in Figure 3.3B. In other words, while the anatomic circuit is present, the electrophysiologic characteristics necessary to activate the circuit are not present. If this patient is placed on a class Ib drug, it is possible to selectively decrease the refractory period of pathway B, giving this circuit the characteristics shown in Figure 3.3A. In other words, the antiarrhythmic drug may make a sustained tachycardia more likely to occur. A similar scenario may develop if a class Ia drug is used in a patient with a circuit resembling the one shown in Figure 3.3C. By increasing the refractory period of pathway B, the benign circuit may be converted to a potentially malignant one. To say it another way, when we administer an antiarrhythmic drug we may be just as likely to increase, as we are to decrease, the tachycardia zone within a potential reentrant circuit — and thus make a sustained arrhythmia more likely instead of less likely. The phenomenon just described is proarrhythmia, or arrhythmia exacerbation. Although proarrhythmia is a common occurrence, it was until recently only poorly recognized by many physicians who use antiarrhythmic drugs. Failing to recognize that drug therapy is actually worsening arrhythmias, frequently leads to inappropriate therapy (such as increasing or adding to the offending drug) and sometimes leads to death. Herein lies the problem with considering antiarrhythmic drugs to be simply arrhythmia suppressants. Proarrhythmia is an inherent property of antiarrhythmic drugs; the mechanism that controls reentrant arrhythmias is the same mechanism that can worsen arrhythmias. Unfortunately, whether a drug will improve or worsen an arrhythmia is difﬁcult to predict before actually administering the drug. Proarrhythmia, therefore, is a possibility for which one must be vigilant whenever using antiarrhythmic drug therapy.

28

I Disorders of the Heart Rhythm: Basic Principles

3 Treatment of Arrhythmias

29

Drug toxicity

Proarrhythmia is probably the most important, and is certainly the most universal, type of toxicity seen with antiarrhythmic drugs. The form of proarrhythmia just mentioned, i.e., the worsening of reentrant arrhythmias, can be seen with any class of antiarrhythmic drugs. In addition, certain antiarrhythmic drugs can produce a second type of proarrhythmia called torsade de pointes. Torsade de pointes (which is discussed in more detail in Chapter 7), is a polymorphic, pausedependent ventricular tachycardia that is associated with prolongation of the QT interval and the subsequent development of triggered activity. (Triggered activity was described brieﬂy in Chapter 2.) Torsade commonly causes syncope and can cause sudden death. It is seen in a subset of otherwise normal individuals — probably 3% to 4% of the population at large — who are prone to develop triggered activity whenever something acts to prolong their cardiac action potentials. Thus, antiarrhythmic drugs in class Ia and class III tend to cause torsade in such individuals. Table 3.3 lists the relative risk of drug-induced proarrhythmia of both types for the various antiarrhythmic drugs. Even aside from proarrhythmia, antiarrhythmic drugs as a group are relatively toxic and poorly tolerated. Table 3.4 lists some of the common side effects of antiarrhythmic drugs. Amiodarone, a class III drug, deserves special recognition as a drug that is uniquely toxic not only among antiarrhythmic drugs but also among all drugs used legally in the United States. Amiodarone has a singular spectrum of toxicities that can be subtle in onset and difﬁcult to recognize and to treat: it can affect virtually every organ system, is accumulated slowly in many organs (toxicity may be related to cumulative lifetime dose), and its half-life may be as long as 100 days. The only reason amiodarone is used, given this toxic potential, is that it is the most efﬁcacious drug yet developed for the treatment of serious cardiac arrhythmias. In carefully selected patients, the use of amiodarone is appropriate and quite helpful.

䉳

Fig. 3.3 Effect of antiarrhythmic drugs on a reentrant circuit. (A) A prototype reentrant circuit (same as described in Figs. 2.5 and 2.6). (B) Changes that may occur with administration of a class la drug. The refractory period of pathway B may be sufﬁciently prolonged by the drug to prevent reentry from occurring. (C) Changes that may occur with administration of class lb drug. The refractory period of pathway B may be shortened, so that the refractory periods of pathways A and B are now nearly equal. A premature impulse would now be more likely to either conduct or block down both pathways, thus preventing the initiation of reentry.

30

I Disorders of the Heart Rhythm: Basic Principles Table 3.3 Relative Risk of Drug-Induced Proarrhythmia.

Drug Class Ia Quinidine Procainamide Disopyramide Class Ib Lidocaine Mexiletine Phenytoin Class Ic Flecainide Propafenone Moricizine Class III Amiodarone Bretylium Sotalol Ibutilide Dofetilide

Risk of Exacerbation of Reentry

Risk of Torsade de Pointes

++ ++ ++

++ ++ ++

+ + +

0 0 0

+++ +++ +++

0 0 +

+ + + + +

+ + +++ +++ +++

Because of the problems associated with the use of antiarrhythmic drugs, as a general rule these drugs should be used only when arrhythmias are signiﬁcantly symptomatic or life-threatening.

Nonpharmacologic therapy Reversing the underlying cause for arrhythmias

The treatment of cardiac arrhythmias should always begin with an attempt to identify and treat reversible etiologies for the arrhythmias. To those etiologies already listed (including electrolyte and acid–base disturbances, ischemia, and pulmonary disorders), we must now add antiarrhythmic drugs. A patient with recurrent arrhythmias who is on antiarrhythmic drug therapy should be regarded in the same way as a patient with fever of unknown origin who is on antibiotic therapy — strong consideration should be given to stopping the drug and reassessing the baseline state. Stopping antiarrhythmic drugs will often improve the frequently recurring arrhythmias.

3 Treatment of Arrhythmias

31

Table 3.4 Common Side Effects of Antiarrhythmic Drugs. Hypotension IV procainamide IV quinidine IV phenytoin IV bretylium

Negative inotropy β blockers ﬂecainide disopyramide

Bradycardia β blockers calcium blockers amiodarone

CNS effects all class Ib amiodarone β blockers ﬂecainide

GI effects all drugs, especially quinidine, procainamide, & class Ib

Hepatic effects amiodarone phenytoin

Pneumonitis amiodarone tocainide

Blood dyscrasias quinidine tocainide phenytoin

Autonomic effects disopyramide quinidine β blockers digitalis sotalol

Other notable toxicities procainamide — drug-induced lupus amiodarone — peripheral neuropathy, proximal myopathy, skin discoloration, skin photosensitivity, hypothyroidism, hyperthyroidism disopyramide — urinary hesitancy CNS, central nervous system; GI, gastrointestinal.

Surgical and ablation therapy

Surgical procedures are frequently helpful in the treatment of arrhythmias. Arrhythmias due to cardiac ischemia often respond to coronary artery bypass surgery. The location of reentrant circuits can be mapped (especially those due to AV bypass tracts and to ventricular tachycardias associated with a discrete ventricular aneurysm), and the reentrant circuit can be disrupted surgically. Transcatheter ablation in the electrophysiology laboratory has largely supplanted most types of arrhythmia surgery and is extremely useful in the management of supraventricular tachyarrhythmias. (Transcatheter ablation will be discussed in detail in Chapter 8.) All these procedures carry at least some risk of complications. Device therapy

Permanent artiﬁcial pacemakers are the mainstay of treatment for bradyarrhythmias. Permanent pacemakers consist of a source of electrical current that is attached to cardiac muscle (usually to ventricular

32

I Disorders of the Heart Rhythm: Basic Principles

muscle) by a wire (lead) and is under the control of an integrated circuit (a small computer). If the heart is not generating intrinsic electrical impulses often enough, the pacemaker sends an electrical current down the lead to stimulate the heart. The current depolarizes the cardiac cells at the tip of the lead (i.e., an action potential is generated), and that depolarization propagates across the myocardium in the normal fashion. Pacemakers today are increasingly sophisticated and complex. Many features are now programmable, such as the rate of pacing and the energy used with each impulse. Pacemakers are available that guarantee the normal sequence of AV contraction with each heartbeat. Other pacemakers can use some physiologic variable (such as the patient’s level of exercise) to judge the optimal heart rate from moment to moment and vary the rate of pacing accordingly. Selecting the appropriate pacemaker for a patient requires extensive knowledge of the technology available. Devices are also useful for patients with tachyarrhythmias. Many patients with malignant ventricular tachyarrhythmias are now being offered the automatic implantable cardioverter–deﬁbrillator (ICD). This device monitors the heart rhythm constantly and, if a potentially lethal tachyarrhythmia occurs, will automatically deliver a large deﬁbrillating current (shock) to the heart to terminate the arrhythmia. The implantable deﬁbrillator has prevented sudden death in thousands of patients who have lethal ventricular arrhythmias. The use of these devices, however, can be difﬁcult and patient selection less straightforward than it might be. (This is discussed in detail in Chapter 7.)

PA R T II

The Electrophysiology Study in the Evaluation and Therapy of Cardiac Arrhythmias

CHAPTER 4

Principles of the Electrophysiology Study

The electrophysiology study can be helpful in evaluating a broad spectrum of cardiac arrhythmias. It can help with assessing the function of the SA node, the AV node, and the His-Purkinje system; with determining the characteristics of reentrant arrhythmias; with mapping the location of arrhythmogenic foci for potential ablation; and with evaluating the efﬁcacy of antiarrhythmic drugs and devices. One might expect a test that can accomplish all this to be extraordinarily complex. On the contrary (although electrophysiologists may not like to admit it), the electrophysiology study is performed by doing two simple things: Recording the heart’s electrical signals, and pacing from localized areas within the heart. Using the information obtained from these relatively simple tasks and keeping in mind the concepts outlined in Part I, one can assess and decide on treatment for a wide array of heart rhythm disturbances. In this chapter, we introduce the principles used in performing the electrophysiology study.

Recording and pacing To discuss intracardiac recording and pacing, we need to introduce two terms that are used by electrophysiologists relating to time measurements. Time measurements are reported in milliseconds (msec, one thousandth of a second), the basic unit of time in electrophysiology. Cycle length

When electrophysiologists talk about heart rate, they typically speak in terms of cycle length — the length of time between each heartbeat (Figure 4.1A). Thus, the faster the heart rate, the shorter the cycle length: An arrhythmia with a rate of 100 beats/min has a cycle length of 600 msec, 35

36

II Electrophysiology Testing for Cardiac Arrhythmias

while an arrhythmia with a rate of 300 beats/min has a cycle length of 200 msec. Nonelectrophysiologists must pay close attention when discussing heart rate with electrophysiologists, to avoid some amusing miscommunications. Coupling interval

When using a pacemaker to introduce a premature impulse, the coupling interval is the time between the last normal impulse and the premature impulse (Figure 4.1B). With earlier premature impulses, the coupling interval is shorter; with later premature impulses, the coupling interval is longer. The electrode catheter

The electrophysiology study is performed by inserting electrode catheters into blood vessels and positioning these catheters in strategic locations within the heart. Once in position, the catheters can be used to perform the two essential tasks of the electrophysiology study: Recording the heart’s electrical signals and pacing.

Fig. 4.1 Time measurements in the electrophysiology laboratory. This ﬁgure depicts pacing from the right ventricular apex. (A) Cycle length is the interval of time between heartbeats during either incremental pacing (as in this ﬁgure) or a spontaneous rhythm. The cycle length of the incrementally paced beats in (A) is 600 msec. (B) Coupling interval is the interval of time between the last normal beat and a premature impulse. In this ﬁgure, the normal beats are represented by eight incrementally paced beats at a cycle length of 600 msec. Following the last incrementally paced beat, a single premature stimulus is delivered with a coupling interval of 250 msec.

4 Principles of the Electrophysiology Study 37

Electrode catheters consist of insulated wires; at the distal tip of the catheter (the end inserted into the heart [Figure 4.2]), each wire is attached to an electrode, which is exposed to the intracardiac surface. At the proximal end of the catheter (the part not inserted into the body [Figure 4.3]), each wire is attached to a plug, which can be connected to an external device (such as a recording device or an external pacemaker). With the exception that they usually have more than two electrodes, these catheters are similar to many temporary pacemaker catheters used in emergency rooms and coronary care units. The catheter shown in Figures 4.2 and 4.3 is a quadripolar electrode catheter, the type most commonly used in electrophysiology studies. Recording intracardiac electrograms

The recording made of the cardiac electrical activity from an electrode catheter placed in the heart is called an intracardiac electrogram. The intracardiac electrogram is essentially an ECG recorded from within the heart. The major difference between a body surface ECG and an intracardiac electrogram is that the surface ECG gives a summation of

Fig. 4.2 The tip of a quadripolar electrode catheter. The electrodes are numbered 1 through 4, the distal (tip) electrode being number 1. The spacing between electrodes is 1 cm.

Fig. 4.3 The proximal end of a quadripolar electrode catheter. The number on each plug corresponds to the appropriate electrode at the tip of the catheter.

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II Electrophysiology Testing for Cardiac Arrhythmias

the electrical activity of the entire heart, whereas the intracardiac electrogram records only the electrical activity of a localized area of the heart — the cardiac tissue located near the electrodes of the electrode catheter. In general, the intracardiac electrogram records the electrical activity between two of the electrodes (i.e., an electrode pair) at the tip of the catheter. This is called a bipolar recording conﬁguration. The intracardiac electrogram is ﬁltered electronically, so that in general only the rapid depolarization phase of the cardiac tissue (corresponding to phase 0 of the action potential) is recorded. Figure 4.4 shows an intracardiac electrogram recorded from a catheter in the right atrium during normal sinus rhythm. As the wave of depolarization spreading outward from the SA node passes by the catheter, a discrete highfrequency, high-amplitude signal is recorded. This signal indicates the precise moment at which myocardial depolarization occurs at the electrode pair which is being used for recording. By having catheters positioned in several different intracardiac locations, one can accurately measure the conduction time from one location to another. Further, if enough catheter positions are used, one can map the sequence of myocardial depolarization as an electrical impulse traverses the heart. In summary, the deﬂection recorded from the electrode catheter represents depolarization of the cardiac tissue in the immediate vicinity

Fig. 4.4 Surface ECG and intracardiac electrogram recorded from the high right atrium (RA) during sinus rhythm. The deﬂection recorded on the RA electrogram reﬂects the precise moment at which the portion of the right atrium at the tip of the electrode catheter is being depolarized.

4 Principles of the Electrophysiology Study

39

of the catheter’s electrodes. Thus, the intracardiac electrogram gives precise, localized data on the heart’s electrical impulse. Pacing

The electrode catheter is also used for pacing. To pace, a pulse of electrical current is carried by the electrode catheter from an external pacemaker to the intracardiac surface, where it causes cardiac cells near the catheter’s electrodes to depolarize. The depolarization of these cardiac cells is then propagated across the heart, just as an electrical impulse arising in the SA node is propagated. Thus, to pace is to artiﬁcially generate a cardiac impulse. By careful positioning of the electrode catheter, one can initiate electrical impulses from almost any desired intracardiac location. During the electrophysiology study, pacing is used to introduce premature electrical impulses, delivered in predetermined patterns and at precisely timed intervals. Such pacing is called programmed stimulation. There are several reasons for performing programmed stimulation. Precisely timed premature impulses allow us to measure the refractory periods of cardiac tissue. By introducing premature impulses in one location and recording electrograms in other locations, one can assess the conduction properties of the intervening cardiac tissue and the pattern of myocardial activation. Programmed stimulation can also help to assess the automaticity of an automatic focus and to study the presence and characteristics of reentrant circuits. Programmed stimulation consists of two general types of pacing: Incremental and extrastimulus pacing (Figure 4.5). Incremental pacing (or burst pacing) consists of introducing a train of paced impulses at a ﬁxed cycle length. The incremental train may last for a few beats or for several minutes. The extrastimulus technique consists of introducing one or more premature impulses (called extrastimuli), each at its own speciﬁc coupling interval. The ﬁrst extrastimulus is introduced at a coupling interval timed either from an intrinsic cardiac impulse or from the last of a short train of incrementally paced impulses. (This train is usually eight beats in duration, owing to tradition rather than to scientiﬁc reasons.) The generally accepted nomenclature for the extrastimulus technique is illustrated in Figure 4.5. The term S1 (stimulus 1) is used for the incrementally paced impulses or the intrinsic beat from which the ﬁrst extrastimulus is timed; S2 is used for the ﬁrst programmed extrastimulus; S3 stands for the second programmed extrastimulus, and so on. This nomenclature (in which, e.g., the number 2 is attached to the ﬁrst extrastimulus) causes a lot of confusion among the uninitiated.

40

II Electrophysiology Testing for Cardiac Arrhythmias

Fig. 4.5 Extrastimulus and incremental pacing. Right ventricular pacing is depicted. (A) Extrastimulus pacing consists of introducing one or more extrastimuli either during the patient’s spontaneous rhythm or (as depicted here) following a train of impulses delivered at a ﬁxed cycle length. This panel shows a single extrastimulus. The ﬁxedcycle-length impulses from which the extrastimuli are timed are referred to as the S1 beats. The ﬁrst extrasimulus is labeled S2. (B) Same as in (A), except that a second extrastimulus is delivered (labeled S3). (C) Same as in (A) and (B), except that a third extrastimulus is delivered (labeled S4). (D) Incremental pacing consists of a train of paced impulses at a ﬁxed cycle length. The S1 beats in (A) through (C) are incrementally paced impulses.

Performance of the electrophysiology study The physical setup of the electrophysiology laboratory

The electrophysiology study is a type of heart catheterization, and much of the equipment necessary for electrophysiologic testing can be found in a general cardiac catheterization laboratory. This includes a ﬂuoroscopic unit, a radiographic table, a physiologic recorder, oscilloscopes, instrumentation for gaining vascular access, and emergency equipment. Equipment required speciﬁcally for electrophysiologic testing includes a programmable stimulator, a multichannel lead switching box (a junction box), and electrode catheters. An arrangement for a typical electrophysiology laboratory is shown in Figure 4.6. The programmable stimulator is a specialized pacing unit built especially for electrophysiology studies. It has the capability of introducing complex sequences of paced beats with an accuracy of within 1 msec. It can also synchronize pacing to the intrinsic heart rhythm and can pace multiple intracardiac sites simultaneously.

4 Principles of the Electrophysiology Study

41

Fig. 4.6 Schematic for the layout of a typical electrophysiology laboratory.

The junction box allows the laboratory personnel to control the connections from the electrode catheters to the various recording and pacing devices. With a series of switches, multiple electrode pairs from multiple catheters can be sorted out for recording and pacing. The physiologic recorder should have enough channels to process three or four surface ECG leads and multiple intracardiac leads (often up to 12). Most electrophysiology laboratories today are equipped with specialized physiologic recorders designed speciﬁcally for electrophysiology studies. Such recorders are computer-based and provide features such as color-coded intracardiac leads, electronic calipers for precise measurements, and hard-disk storage of the entire study. Equipment to deal with cardiac emergencies is essential especially because many electrophysiology studies include the intentional induction of arrhythmias that can cause hemodynamic collapse. This includes a deﬁbrillator, a full complement of cardiac medications, and

42

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equipment for maintaining airway support. Likewise, enough trained personnel should always be present to deal with any cardiac emergency. As a minimum, this should include the electrophysiologist, two cardiac nurses who are trained in electrophysiologic procedures (or one nurse and a second physician), and a technician. Preparation of the patient

Although preparation of the patient will vary somewhat depending on the nature of the study to be performed, all patients having electrophysiology studies should be given a clear understanding of the purpose and nature of the procedure and the potential beneﬁts and risks. As with any procedure in medicine, the patient should sign a statement of informed consent prior to the study. Ideally, the electrophysiologic evaluation should be performed while the patient is in a baseline state — nonessential drugs should be withdrawn (especially antiarrhythmic agents), any cardiac ischemia or heart failure maximally treated, electrolytes controlled, and every effort made to prevent excessive anxiety — which can cause excessive sympathetic tone. Anxiety is most easily kept to an acceptable level by adequately preparing the patient for what to expect in the electrophysiology laboratory. Any cardiac catheterization procedure can cause potentially dangerous arrhythmias, but patients having electrophysiology studies especially need to be aware of this possibility. In particular, patients who are having studies for known or suspected ventricular tachyarrhythmias should be psychologically prepared for the possibility that induction of an arrhythmia may produce loss of consciousness and require deﬁbrillation. Fortunately, the efﬁcacy of electrophysiologic testing and the remarkable safety record achieved in most laboratories go a long way toward allaying the fears of most patients and their families. Detailed discussions with the patient serve not only to guarantee truly informed consent but also to alleviate the patient’s anxiety and build his or her conﬁdence in the electrophysiologist. Insertion and positioning of electrode catheters

The patient is brought to the catheterization laboratory in the fasting state, and the catheterization sites are prepared and draped. The majority of electrophysiology studies can be performed from the venous side of the vascular system, thus precluding the necessity of catheterizing the arterial tree. Under sterile conditions and after local anesthesia is given, catheters are inserted in most instances percutaneously by the modiﬁed Seldinger technique (a needle-stick technique that does not

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require a cutdown). Only extremely rarely do patients need to be placed under general anesthesia to perform an electrophysiology study; however, premedication with a benzodiazepine is sometimes used in patients who are extremely anxious. Most often, catheters are inserted into the femoral veins (two catheters can safely be inserted into the same femoral vein). Catheters are inserted from the upper extremities either for more complicated studies, which require multiple catheters; when there is a contraindication to the use of the femoral veins; when a catheter will be left in place at the end of the procedure; or when positioning of the catheter is easier from the upper extremities (such as in coronary sinus catheterization). In these cases, the internal or external jugular veins, the subclavian veins, or the brachial veins may be used. In those instances where access to the left ventricle is required, the femoral arterial approach is used most often. In many laboratories, a small catheter is routinely inserted into an artery for continuous monitoring of blood pressure. Under ﬂuoroscopic guidance, the catheters are placed into the proper intracardiac positions. For a simple diagnostic study, generally one catheter is positioned in the high right atrium and the second catheter is placed in the His position (described later). One of these catheters can later be moved to the right ventricle if ventricular pacing is required. For studies of supraventricular tachycardias, additional catheters are commonly placed in the right ventricle and the coronary sinus (thus allowing recordings from all four major cardiac chambers and from the His position). In the right atrium, catheters are most commonly positioned in the high lateral wall, near the junction of the superior vena cava. This position approximates the location of the SA node and is the region of the atrium that is depolarized earliest during normal sinus rhythm. Pacing from this area results in P wave conﬁgurations that are similar to normal sinus beats. Pacing and recording from the left atrium are usually accomplished by inserting an electrode catheter into the coronary sinus (Figure 4.7). The os of the coronary sinus lies posterior and slightly inferior to the tricuspid valve and is most easily entered from a superior approach (i.e., from the upper extremities). The coronary sinus itself lies in the AV groove — that is, between the left atrium and the left ventricle. Thus, deﬂections from both the left atrium and the left ventricle are easily recorded from a catheter positioned in the coronary sinus. Pacing the left atrium from the coronary sinus is accomplished routinely — only rarely can the left ventricle be paced from this position. Although a patent foramen ovale will sometimes allow direct entry into the left

44 II Electrophysiology Testing for Cardiac Arrhythmias

Fig. 4.7 A catheter positioned in the coronary sinus can record left atrial and left ventricular electrograms because the coronary sinus lies in the AV groove between the left atrium and the left ventricle. AVN, AV node; CS, coronary sinus; EC, electrode catheter; FS, ﬁbrous skeleton of the heart; HIS, His bundle; IVC, inferior vena cava; MV, mitral valve; OS, os of the coronary sinus; RA, right atrium; RV, right ventricle; SVC, superior vena cava; TV, tricuspid valve.

atrium, we prefer to use the coronary sinus to avoid the slight possibility of causing an embolus in the systemic circulation. Electrode catheters in the right ventricle are usually positioned in the apex for recording and the apex or the outﬂow tract for pacing. Placing electrode catheters in the left ventricle is not part of the standard electrophysiology study. When it is necessary to do so (e.g., when

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ablation procedures require access to the left ventricle or left atrium), vascular access is usually gained through one of the femoral arteries; although some electrophysiologists have become adept at entering the left side of the heart transseptally from the right atrium. The His bundle electrogram is the recording that gives the most information about AV conduction. To record the His bundle electrogram, an electrode catheter is passed across the posterior aspect of the tricuspid valve (near the penetration of the His bundle into the ﬁbrous skeleton [Figure 4.8]). The catheter is maneuvered while continuously recording electrograms from several electrode pairs (so that the best pair for recording can be selected), until an electrogram similar to the one shown in Figure 4.8 is seen. The electrode pair that records the His electrogram is thus placed in a strategic location. It straddles the important structures of the AV conduction system and allows one to record the electrical activity of the low right atrium, the AV node, the His bundle, and a portion of the right ventricle — all from one electrode pair. Once the catheters are in position, the various electrode pairs are set up for recording and pacing. The leads recorded include various surface ECG leads and intracardiac electrograms from each electrode catheter. Figure 4.9 shows a typical baseline recording for a typical baseline electrophysiology study, displaying surface ECG leads I, II, and V1 (thus providing a lateral, an inferior, and an anterior lead from which to assess the QRS axis) as well as leads from two intracardiac catheters (high right atrium and His positions). For ventricular recording and pacing, the right atrial catheter is moved to the right ventricle after atrial pacing is completed. The basic electrophysiology protocol

The protocol used in electrophysiology studies varies according to the speciﬁc type of procedure being performed; but most electrophysiologic procedures follow the same general outline: 1 Measurement of baseline conduction intervals 2 Atrial pacing a. Assessment of SA nodal automaticity and conductivity b. Assessment of AV nodal conductivity and refractoriness c. Assessment of His-Purkinje system conductivity and refractoriness d. Induction of atrial arrhythmias 3 Ventricular pacing a. Assessment of retrograde conduction b. Induction of ventricular arrhythmias 4 Drug testing

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Fig. 4.8 Positioning of the His bundle catheter. The His bundle electrogram is recorded from a catheter that lies across the posterior aspect of the tricuspid valve. Abbreviations are the same as in Figure 4.7. See p. 49 for a description of “A”, “H” and “V” spikes on the His electrogram.

Chapters 5, 6, and 7 discuss the individual steps of the electrophysiology study in detail. Before proceeding to speciﬁcs, however, we need to review the principles of how one can evaluate the electrophysiologic properties of the heart and assess and treat reentrant arrhythmias from the simple expediency of recording and pacing from intracardiac electrodes.

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Fig. 4.9 Typical baseline recording of intracardiac electrograms. In this ﬁgure, one surface ECG lead is shown, as well as intracardiac electrograms from the high right atrium (RA), His bundle, coronary sinus, and right ventricular apex. Conduction intervals are as follows: BCL (basic cycle length) is the interval between successive A waves (measured from the RA catheter); PR interval is the time from the beginning of the P wave to the beginning of the QRS complex (measured from the surface ECG); QRS duration is the width of the QRS complex on the surface ECG; IACT (intraatrial conduction time) is the interval from the SA node to the AV node and is measured from the beginning of the P wave on the surface ECG to the A deﬂection on the His bundle electrogram. The AH and HV intervals are discussed in detail in the text (see p. 49).

Evaluation of the electrophysiologic properties of the heart By recording and pacing from electrode catheters, one can evaluate the fundamental electrophysiologic properties of the heart — namely, automaticity, conduction velocity, and refractory periods. Automaticity

The electrophysiology study can be used to assess the normal automaticity of the SA node, thanks to the phenomenon known as overdrive suppression. An automatic focus such as the SA node can be overdriven by a

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more rapidly ﬁring pacemaker. This means that the more rapid pacemaker depolarizes the SA node faster than it can be depolarized by its intrinsic automaticity. When the overdriving pacemaker stops, there is often a relatively long pause before the SA node recovers and begins depolarizing spontaneously again. The pause induced in an automatic focus by a temporarily overdriving pacemaker is called overdrive suppression. Overdrive suppression of the SA node is accomplished in the electrophysiology laboratory by pacing the atrium rapidly (thus overdriving the SA node), then suddenly turning off the pacemaker, and measuring how long it takes for the SA node to recover. A diseased SA node tends to have a grossly prolonged recovery time after overdrive pacing. The evaluation of SA nodal dysfunction is covered in detail in Chapter 5. Overdrive suppression of automatic foci is also clinically relevant when patients are dependent on subsidiary escape pacemakers to sustain life (e.g., patients with complete heart block and ventricular escape rhythms). These subsidiary pacemakers are automatic foci like the SA node and are thus subject to overdrive suppression. If such a patient receives a temporary pacemaker and after a time the temporary pacemaker suddenly loses capture (as temporary pacemakers sometimes do), the patient may be left with a prolonged, possibly fatal asystolic episode due to overdrive suppression of the escape pacemaker. In such patients, careful positioning of the temporary pacemaker to guarantee excellent pacing thresholds in a very stable location is essential, and every precaution must be taken to keep the temporary lead stable (such as enforced bed rest) until a permanent pacemaker can be inserted. Tachyarrhythmias due to abnormal automaticity (such as automatic ventricular tachycardia due to ischemia) do not lend themselves well to study in the electrophysiology laboratory. Overdrive suppression of such abnormal automatic foci is not a prominent feature and usually cannot be demonstrated. Also, as we have already discussed, automatic arrhythmias cannot be induced during electrophysiologic testing. Thus, the evaluation of automatic tachyarrhythmias is not an indication for an electrophysiology study. Conduction velocity

Conduction velocity refers to the speed of conduction of an electrical impulse across the heart and, as we have noted, is related to the rate of rise (i.e., the slope) of the depolarization phase (phase 0) of the action potential. By measuring the time it takes for an electrical impulse to travel from one intracardiac location to another (referred to as a conduc-

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tion interval), one can use electrode catheters to assess the conduction velocities of various portions of the cardiac electrical system. The best example of measuring conduction velocity from intracardiac electrograms is given by the His bundle electrogram. As noted previously, this electrogram contains signals from all the critical structures of the AV conducting system. Figure 4.8 represents the His bundle electrogram from a patient in normal sinus rhythm. As shown, the His electrogram contains three major deﬂections. The ﬁrst deﬂection is the A spike. This deﬂection represents depolarization of the tissue in the low right atrium, just as the electrical impulse enters the AV node. Once in the AV node, the impulse encounters tissue that depolarizes slowly. (As discussed in Chapter 1, the slow depolarization of the AV nodal tissue is a result of the lack of rapid sodium channels in AV nodal cells). Because the depolarization of the AV node is slow, no high-frequency signal is generated, and the passage of the impulse through the AV node does not produce a deﬂection on the His bundle electrogram. When the impulse exits the AV node and zips down the His bundle (again encountering rapidly depolarizing cells), the His bundle deﬂection (i.e., the H spike) is produced on the electrogram. As the impulse passes distally through the bundle branches and on to the farther reaches of the Purkinje system, it moves away from the recording electrode pair. Because of their distance from the recording electrodes, the Purkinje ﬁber depolarizations are not recorded on the His electrogram (although the right bundle branch depolarization is sometimes seen). Finally, as the impulse is spread to the ventricular myocardium, the depolarization of the ventricular muscle near the His catheter produces the V deﬂection on the His electrogram. By analyzing the deﬂections on the His bundle electrogram, the conduction properties of the major structures of the AV conduction system can be deduced. The conduction interval from the beginning of the A deﬂection to the beginning of the H deﬂection (the AH interval) represents the conduction time through the AV node (normally 50 to 120 msec). The interval from the beginning of the H deﬂection to the beginning of the V deﬂection (the HV interval) represents the conduction time through the His-Purkinje system (normally 35 to 55 msec). Disease in the AV node will often produce a prolongation in the AH interval, whereas disease in the distal conducting system produces a prolongation in the HV interval. The AH and HV intervals are two of the basic conduction intervals measured at the beginning of the electrophysiology study. Other basic conduction intervals (shown in Figure 4.9) include the basic cardiac cycle length, the QRS duration, the PR interval, and the intraatrial

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conduction interval. The basic cycle length is the interval between successive atrial impulses as measured in the right atrial catheter (in order to approximate the basic rate of depolarization of the SA node). The PR interval is measured from the surface ECG leads and is deﬁned as the interval from the beginning of the P wave to the beginning of the QRS complex. The QRS duration, the interval from the beginning of the QRS complex to the end of the QRS complex, is also measured from the surface ECG leads. The intraatrial conduction interval approximates the conduction time from the sinus node to the AV node and is measured from the beginning of the P wave on the surface ECG to the beginning of the A spike on the His bundle electrogram. Note that the intraatrial conduction interval, the AH interval, and the HV interval, are the three basic components of the PR interval. Depending on the type of electrophysiology study being performed and the type of information needed, other conduction intervals may be measured, such as retrograde conduction intervals (from the ventricle to the atrium). Refractory periods

Thus far, we have deﬁned the refractory period as the period of time after depolarization during which a cell cannot be depolarized again, and we have related the refractory period of a cell to the duration of the action potential. Because we cannot measure a cell’s action potential duration in the electrophysiology laboratory, the refractory period must be redeﬁned in such a way as to make it meaningful in the laboratory setting. Thus, the refractory period of cardiac tissue is deﬁned in terms of the tissue’s response to premature paced impulses. Here, electrophysiologists have outdone themselves by deﬁning three different kinds of refractory periods: The effective refractory period, the relative refractory period, and the functional refractory period. The effective refractory period (ERP; Figure 4.10) is the deﬁnition that most closely coincides with our original deﬁnition of the refractory period. When introducing a premature impulse, that impulse will fail to propagate through tissue that is refractory. The ERP of a tissue is the longest coupling interval for which a premature impulse fails to propagate through that tissue. In other words, the ERP refers to the latest early impulse that is blocked — if the premature impulse were any later, the tissue would be recovered and would propagate the impulse. In general, the end of ERP occurs sometime during the last third of phase 3 of the action potential. The relative refractory period (RRP; Figure 4.10) requires the introduction of a new concept. Recovery from refractoriness turns out to be a

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Fig. 4.10 Effective and relative refractory periods. During the effective refractory period (ERP), the cell cannot be depolarized. During the relative refractory period (RRP), the cell can be depolarized, but the resultant action potential displays slower phase 0 activity (dotted lines).

gradual process instead of an instantaneous one. As shown, the end of the ERP occurs during phase 3, before a cell is fully repolarized (that is, before phase 4 begins). If a cardiac cell is stimulated after the end of the ERP but before the cell is fully repolarized, the resulting action potential has a slower upstroke (phase 0) and therefore propagates at a slower conduction velocity. The period of time from the end of the ERP to the beginning of phase 4 is called the RRP. Formally, the RRP of a tissue is the longest coupling interval for which a premature impulse results in slowed conduction through that tissue. At the end of the RRP, the tissue is fully recovered. At least the ERP and RRP can be related in some way to the duration of the action potential. The functional refractory period (FRP) loses even that relationship to our original notion of “refractory period”. The FRP of a tissue is the smallest possible time interval between two impulses that can be conducted through that tissue. The FRP is a measure of the output of a tissue. Think of a tiny electrophysiologist standing on the His bundle with a stopwatch, determined to measure the FRP of the AV node. A larger electrophysiologist is pacing the atrium with progressively earlier (i.e., more premature) impulses. The only thing our miniature friend can detect, however, is each electrical impulse exiting the AV node and zipping down the His bundle (don’t worry — he is wearing rubber-soled shoes). Each time an impulse exits the AV node and stimu-

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lates the His bundle, the tiny electrophysiologist records the time interval since the previous impulse. Eventually, premature impulses stimulating the AV node are so premature that the ERP of the AV node is reached (i.e., the impulse is blocked when it reaches the AV node), and therefore no more impulses are transmitted to the His bundle. The FRP of the AV node is the shortest interval between successive impulses observed by our tiny timer. What possessed electrophysiologists to invent such a thing as the FRP? First, since the FRP of a tissue is determined by transmission of impulses through that tissue, FRP is a measurement of both refractoriness and conduction velocity of a tissue. As shown in the discussion of RRP, refractoriness and conduction velocity are intimately related at narrower coupling intervals. The FRP is a way of quantifying this relationship. Second, the FRP may be clinically relevant more often than the more straightforward types of refractory periods. The best example is in atrial ﬁbrillation, in which much effort is often spent in slowing the ventricular response. The drugs used for this purpose tend both to increase refractoriness and to slow conduction in the AV conducting system. One of the best measures of effective therapy, then, is the narrowest interval between successive QRS complexes (i.e., the FRP of the AV conducting system). Third, when inventing a list of anything (such as types of refractory periods), it is best to have at least three items on the list. The effect of cycle length and autonomic tone on refractory periods and conduction velocity

The refractory period of cardiac tissue is affected by the cycle length. For most tissue, shorter cycle lengths (i.e., faster heart rates) decrease refractory periods. The glaring exception to this general rule is the AV node, in which shorter cycle lengths increase refractory periods. Autonomic tone affects both refractory periods and conduction velocity. An increase in sympathetic tone increases the conduction velocity and decreases the refractory periods throughout the heart. An increase in parasympathetic tone decreases the conduction velocity and increases the refractory periods. Here again, there is a differential effect on the AV node, which is far more richly supplied by parasympathetic ﬁbers than most of the heart is. Thus, parasympathetic tone has a disproportionate effect on the AV node.

Evaluation of reentrant arrhythmias The ability to induce and terminate reentrant arrhythmias renders them amenable to detailed study. Consequently, the electrophysiology study

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has become vitally important in the evaluation and treatment of reentrant tachyarrhythmias. Although the techniques used to study different types of reentrant arrhythmias vary (this will be discussed in detail in Chapters 6 and 7), the principles behind the electrophysiologic evaluation of all types of reentry are the same. Programmed stimulation in reentrant arrhythmias

The hallmark of the reentrant mechanism is the ability to induce and terminate the arrhythmia with programmed pacing techniques. Figure 2.6 shows the basic principle behind inducing a reentrant arrhythmia. A paced premature impulse enters the reentrant loop at a critical coupling interval, when pathway B is still refractory from the previous impulse (i.e., the premature impulse arrives during the ERP of pathway B) — but after the ERP of pathway A, which accepts the early impulse. Note that, if the impulse enters pathway A during its RRP, the requirement for slow conduction down pathway A may be met automatically (since by deﬁnition conduction is slow during the RRP). Because of the slow conduction down pathway A, pathway B has time to recover and accepts the premature impulse in the retrograde direction. Reentry is established. Once a reentrant arrhythmia is established, premature paced impulses encountering the loop can do one of three things (Figure 4.11). First, the early impulse may encounter refractory tissue, which prevents it from entering the circuit (Figure 4.11A). In this case, the premature beat will not affect the reentrant rhythm. Second, the early paced impulse may enter the loop and conduct down the slow pathway (pathway A) but collide with the reentrant impulse in the fast pathway (Figure 4.11B). In this case, the paced impulse resets the reentrant rhythm. Finally, the early impulse may enter the loop at just the right moment to encounter refractory tissue in pathway A and to collide with the circulating wavefront in pathway B (Figure 4.11C). In this case, the reentrant rhythm is terminated. A paced impulse must reach a reentrant circuit at a critical moment to start or stop an arrhythmia. The ability to arrive at such a critical moment is dependent on several factors, including the distance of the pacing electrode from the reentrant circuit, and the refractoriness and the conduction velocity of the tissue lying between the catheter and the circuit. If the catheter is far away from the reentrant circuit and if the intervening tissue has long refractory periods and slow conduction, it is less likely that a paced impulse will reach the reentrant circuit early enough to either induce or terminate an arrhythmia. For this reason, stimulation protocols usually call for pacing from more than one location, to improve the chances of ﬁnding a location near the reentrant

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circuit. In addition, most stimulation protocols call for coupling up to three or four premature impulses together. The resulting short cycle lengths reduce refractory periods and increase conduction velocity in the intervening tissue, giving subsequent impulses a better chance of reaching the reentrant circuit. Pacing from various locations during supraventricular tachycardia can help to determine whether certain intracardiac locations are part of the reentrant loop. For instance, pacing from a right ventricular site which does not affect a narrow complex tachyarrhythmia is evidence against a macroreentrant tachycardia that includes both atrial and ventricular tissue in the reentrant loop. Chapter 6 discusses this concept in more detail. Recording electrograms during reentrant arrhythmias

By recording intracardiac electrograms during reentrant tachycardias, it is possible to characterize the pathways of large reentrant circuits (present in many supraventricular arrhythmias) or to map the general location of small reentrant circuits (present in most ventricular tachycardias). Especially helpful in the evaluation of supraventricular arrhythmias is the pattern of atrial activation during tachycardia. As will be discussed in Chapter 6, some types of reentrant supraventricular arrhythmias show characteristic patterns of atrial activation. A diagnosis can often be made by analyzing the intracardiac atrial electrograms. By recording multiple ventricular electrograms during induced ventricular tachycardia and looking for the earliest ventricular activation site, the general location of the reentrant circuit can be deduced. By thus mapping the ventricular activation pattern, ablation of the reentrant circuit can be attempted. Effect of autonomic maneuvers, antiarrhythmic drugs, and devices on reentry

The electrophysiology study can help to determine the effect of autonomic maneuvers on reentrant arrhythmias. By manipulating 䉳 Fig. 4.11 Effect of premature impulses on a reentrant arrhythmia. (A) A relatively late premature impulse may encounter refractory tissue that prevents penetration into the reentrant circuit. In this case, reentry is not affected. (B) An earlier premature impulse than depicted in (A) may enter the reentrant circuit and abolish the reentrant impulse in one pathway (pathway B in this ﬁgure) but reestablish reentry by conducting down the opposite pathway (pathway A). In this case, the reentrant rhythm is reset. (C) A very early premature impulse may abolish the reentrant arrhythmia in pathway B, while encountering refractory tissue in pathway A. In this case, reentry is terminated.

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autonomic tone and reassessing the inducibility of arrhythmias, one can determine whether reentrant arrhythmias are dependent on autonomic tone. In supraventricular arrhythmias, reentry which depends on autonomic tone is strong evidence that the AV node is involved in the reentrant loop. Stimulating the ventricle during the infusionofsympathomimeticagentscanhelptodiagnosecatecholaminedependent ventricular tachycardia. Diagnosing this relatively infrequent type of ventricular tachycardia is important because this arrhythmia almost always responds to β blockers. Likewise, the effect of antiarrhythmic drugs on reentrant arrhythmias can be assessed in the electrophysiology laboratory. As discussed in Chapter 3, drugs can ameliorate, exacerbate, or not affect reentrant loops. Programmed stimulation offers a way of predicting the effect of a drug on a reentrant loop before committing a patient to long-term therapy with that drug. Ideally, if a drug has a favorable effect on a reentrant circuit, it will render a previously inducible arrhythmia noninducible. This is the rationale behind serial drug testing in the electrophysiology laboratory. By studying the characteristics of an induced arrhythmia, one can assess the feasibility of using implantable antitachycardia devices to terminate spontaneous arrhythmias. Several considerations are important before considering implantable devices. How many different types of arrhythmias are inducible? What are their cycle lengths? What pacing sequences reliably terminate the induced arrhythmias? Does pacing ever degenerate a hemodynamically stable arrhythmia to an unstable one? Are there benign tachyarrhythmias (such as sinus tachycardia) that may fool a device into delivering inappropriate therapy? How do drugs affect the inducibility, rate, morphology, and terminability of arrhythmias? All these questions can be addressed through careful study in the electrophysiology laboratory.

Complications of electrophysiologic testing On ﬁrst learning about the electrophysiology study — especially when the purpose of that study is to induce lethal ventricular arrhythmias — many physicians assume that a test that sounds so barbaric must be dangerous. On the contrary: The electrophysiology study is remarkably safe, often much safer than the standard cardiac catheterization. The electrophysiology study is a form of heart catheterization, and it necessarily carries the qualitative risks of a heart catheterization. These include cardiac perforation, hemorrhage, thromboembolism, phlebitis, and infection. Because the most common complications of a general

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heart catheterization involve damage to the arterial tree, and because most electrophysiology studies do not require arterial puncture, the statistical risk of serious vascular damage is actually substantially less with the electrophysiology study than with a standard cardiac catheterization. In most laboratories, the cumulative risk of thromboembolism or phlebitis, bacteremia, or hemorrhage requiring transfusion is well below 1%. One might think that a procedure that intentionally induces lethal arrhythmias would entail signiﬁcant mortality. In fact, the risk of death during an electrophysiology study approaches zero. Reentrant ventricular arrhythmias are induced in the electrophysiology laboratory under controlled circumstances. Immediate efforts are made to terminate hemodynamically unstable arrhythmias, and it turns out that these arrhythmias are readily terminable if they are attacked quickly. In most laboratories, the average length of time the patient remains in an induced ventricular tachycardia is less than 30 seconds. Only a small minority of patients with inducible ventricular tachyarrhythmias require DC shocks for termination and the need to initiate cardiopulmonary resuscitation procedures is exceedingly rare.

CHAPTER 5

The Electrophysiology Study in the Evaluation of the SA Node, AV Node and His-Purkinje system

As we saw in Chapter 2, the SA node, AV node, and His-Purkinje system are responsible for generating, propagating and distributing the heart’s electrical impulse, and thus for determining the cardiac rhythm and rate, and for optimizing hemodynamic performance. Speciﬁcally, the SA node continuously regulates the heart rate according to the body’s ﬂuctuating needs; the AV node and His bundle optimize the transmission of the electrical impulse from the atria to the ventricles; and the Purkinje system coordinates the contraction of the left and right ventricles. In this chapter, we will discuss disorders of the SA node, AV node, and His-Purkinje system, emphasizing how (and when) the electrophysiology study can help in their evaluation. Bradycardia is the most common manifestation of abnormal impulse generation and propagation and will be the main focus of this chapter. Tachyarrhythmias can also arise from disorders of the SA node or AV conduction system. With one exception, these will be discussed in Chapter 6. The exception is inappropriate sinus tachycardia (IST), a unique and puzzling arrhythmia which is difﬁcult to classify. Since the one thing we can say for sure about IST is that it manifests as abnormal SA nodal function, we will cover it here. We will also brieﬂy discuss bundle branch block, a disorder of the Purkinje system that causes ventricular discoordination. Finally, we will provide a brief review of pacemaker therapy. In this chapter, the reader will note a recurring theme: While the electrophysiology study has provided us with detailed knowledge of how the SA node, AV node and His-Purkinje system work, now that we have acquired this knowledge, we can usually evaluate patients with disorders of these cardiac structures without actually having to perform an electrophysiology study. Indeed, the original electrophysiologists were 58

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so successful in achieving their prime directive — i.e., understanding how the cardiac impulse is formed and propagated— that they nearly put themselves out of business. Fortunately, a second generation of electrophysiologists quickly ﬁgured out how to apply electrophysiologic testing to the tachyarrhythmias, thus rescuing the profession — but that’s a story for later chapters.

Evaluation of SA nodal abnormalities Anatomy of the SA node

The SA node can be thought of as a subendocardial, comma-shaped structure, approximately 3 mm in width and 10 mm in length, the head of which is located laterally to the right atrial appendage, near the junction of the atrium and the superior vena cava, on the crista terminalis. (The crista terminalis is an endocardial ridge extending like a narrow mountain chain from the superior to the inferior vena cava along the lateral right atrium.) The tail of the SA nodal “comma” extends downward along the crista terminalis, toward the inferior vena cava. The SA node receives rich innervation from both sympathetic and parasympathetic ﬁbers; accordingly, its function is strongly inﬂuenced by the autonomic nervous system. There is some evidence that autonomic tone helps to determine which portion of the SA node (i.e., the head or the tail) is “ﬁring” at a given time — elevated sympathetic tone tends to trigger the head of the SA node, while elevated parasympathetic tone tends to trigger the tail. SA nodal dysfunction

Disease of the SA node is the most common cause of bradycardia. The bradyarrhythmias that accompany SA nodal disease can manifest as intermittent or sustained sinus bradycardia, as sudden episodes of SA nodal arrest or exit block, or as sinus bradycardia alternating with paroxysms of atrial tachyarrhythmias (a condition referred to as brady-tachy syndrome). When sinus bradyarrhythmias are sufﬁcient to produce symptoms, sick sinus syndrome is said to be present. (Note that the “ofﬁcial” deﬁnition of sinus bradycardia can be misleading. While most textbooks deﬁne normal sinus rhythm as having a rate between 60 and 100 beats/min, this range is probably incorrect. Normal, healthy individuals often have resting sinus rates as low as 40; while resting heart rates in the upper 80s or 90s often indicate the presence of occult medical problems, such as anemia or cardiopulmonary or thyroid disorders.)

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Clinical studies show that SA nodal disease is usually benign. Speciﬁcally, the presence of asymptomatic sinus bradyarrhythmias is not associated with early mortality. Thus, the level of aggressiveness that ought to be used in evaluating and treating suspected SA nodal disease is solely dependent on whether any associated symptoms are thought to be present. If SA nodal disease is causing symptoms (i.e., if sick sinus syndrome is present), permanent pacing is indicated. If there are no symptoms, in general there is no indication for pacing. By far the most common etiology of SA nodal disease is simple ﬁbrosis of the SA node; a condition that is associated with aging and often is also accompanied by diffuse ﬁbrosis within the atria and the AV conducting system. Accordingly, most patients with SA nodal dysfunction are elderly. Other causes of SA nodal dysfunction include atherosclerotic disease involving the SA nodal artery; cardiac trauma, especially during surgical correction of congenital heart disease; cardiac inﬁltrative or inﬂammatory disorders; and thyroid disorders. Brady-tachy syndrome deserves a special mention. This syndrome occurs because the diffuse atrial ﬁbrosis that often accompanies SA nodal dysfunction can produce a propensity for atrial ﬁbrillation or ﬂutter. Individuals with brady-tachy syndrome thus will have intermittent episodes of atrial tachyarrhythmias, with intervening periods of sinus bradycardia. Importantly, because their diseased SA nodes often display exaggerated overdrive suppression (see Chapter 4 and below), these patients tend to have very prolonged asystolic pauses when their tachyarrhythmias abruptly terminate. Quite often then their presenting symptoms have little to do directly with either the tachycardia or the sinus bradycardia — instead they are frequently caused by this posttachycardia asystole. Thus, patients with brady-tachy syndrome can have sudden and relatively severe episodes of lightheadedness, or even frank syncope. Furthermore, because the atrial ﬁbrosis also commonly involves the AV conduction system, during their atrial tachyarrhythmias these patients may have surprisingly well-controlled (or even slow) ventricular responses. Seeing an unexpectedly slow ventricular response in a patient with atrial ﬁbrillation should thus immediately raise the question of a generalized disorder of the conducting system — and the physician should be prepared to administer immediate pacing therapy if cardioversion is contemplated. Patients with brady-tachy syndrome often end up with chronic atrial ﬁbrillation accompanied by a reasonably well-controlled ventricular response. Indeed, one might be tempted to view this chronic atrial ﬁbrillation as “God’s way” of guaranteeing an adequate heart rate in the face of diffuse conducting system disease. While this may be so, in the

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intervening years patients are often very symptomatic, not to mention their risk for syncope-induced trauma, so sitting on one’s hands and waiting for this ﬁnal, relatively stable rhythm to occur does not constitute adequate therapy. Although the electrophysiology study can help to document the presence of SA nodal dysfunction, it generally cannot help to assess whether such dysfunction is causing symptoms — or, therefore, whether pacing therapy is indicated. One is, however, occasionally faced with a patient who has symptoms suggesting signiﬁcant bradycardia (such as lightheadedness or syncope), without clearly documented bradycardia. In such circumstances, the electrophysiology study can be helpful in determining whether or not the SA node is intrinsically normal. Evaluating SA nodal function in the electrophysiology laboratory Sinus node recovery time (SNRT)

A primary manifestation of SA nodal dysfunction is disordered automaticity — that is, the slope of phase 4 automaticity is reduced in the SA node, resulting in bradycardia. The test designed to assess SA nodal automaticity in the electrophysiology laboratory is the sinus node recovery time (SNRT; Figures 5.1 and 5.2). Measurement of the SNRT is based on the phenomenon of overdrive suppression. Overdrive suppression is the temporary slowing of automaticity seen when an automatic focus is exposed to rapid, extrinsic electrical stimuli. When this overdriving stimulation stops, it takes the automatic focus a few cycles to recover its normal rate of discharge. Until it recovers, it ﬁres more slowly than its original baseline rate; thus, the automatic focus has been transiently “suppressed” by overdrive stimulation. Overdrive suppression is a normal behavior of automatic foci; in SA nodal disease, however, overdrive suppression tends to be exaggerated. In nature, as we have seen, overdrive suppression of the SA node is caused by atrial tachyarrhythmias. In the electrophysiology laboratory, we provoke it with a temporary pacemaker. Measuring SNRT Measuring the SNRT is simple in concept and in practice; although interpreting the results can be more challenging. An electrode catheter is placed in the high right atrium near the SA node and pacing is initiated to overdrive the SA node. After a while, pacing is terminated and the ensuing “recovery” time from the last paced beat to the next spontaneous sinus beat is measured.

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Fig. 5.1 A normal sinus node recovery time (SNRT). This ﬁgure shows three surface ECG leads (top three tracings), a right atrial (RA) electrogram (fourth tracing), and a His bundle electrogram (ﬁfth tracing). In measuring the SNRT, only the RA electrogram needs to be examined. The ﬁrst three impulses on the RA electrogram represent the ﬁnal three paced beats during 30 seconds of incremental pacing. Pacing is stopped, and the interval from the last paced atrial complex to the ﬁrst spontaneous atrial complex on the RA electrogram is measured. In this instance, the basic cycle length is 800 msec and the SNRT equals 1260 msec. This is a normal value.

Fig. 5.2 An abnormal sinus node recovery time (SNRT). This ﬁgure shows three surface ECG leads and the right atrial (RA) electrogram. The last three paced impulses are shown. The interval following termination of pacing (from the RA electrogram) is 2200 msec, an abnormally long SNRT. Note that during the recovery interval a premature ventricular complex (PVC) is seen. Because this PVC does not conduct retrogradely (this is obvious since no corresponding atrial activity is present on the RA electrogram), the PVC does not affect the sinus node and therefore does not affect measurement of the SNRT.

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In the formal measurement of SNRT several pacing sequences are tested, beginning with a pacing rate just slightly faster than the basic sinus rate, and generally ending with a cycle length of 300 msec (200 beats/min.) Each pacing sequence is maintained for at least 30 seconds to maximize overdrive suppression — and is then abruptly stopped. The ﬁrst recovery interval (the interval from the last paced atrial complex to the ﬁrst spontaneous SA nodal depolarization) is normally longer than the pre-pacing baseline sinus interval, reﬂecting the degree of overdrive suppression induced by pacing. After pacing is stopped, the SA node gradually returns to its baseline rate over ﬁve to six beats. In SA nodal disease, two observations are commonly seen. First, the initial recovery interval can be longer than normal. Second, the gradual return to the baseline sinus rate can be interrupted during subsequent recovery intervals by marked “secondary pauses”. By the end of the study, several initial recovery intervals will have been measured: One at each pacing rate. In addition, one or more secondary pauses may have been observed. The ofﬁcial SNRT is deemed to be the longest recovery interval observed during the entire test; whether it is one of the initial recovery intervals or a secondary pause. One might think that the longest post-pacing recovery times would always be seen after the more rapid pacing rates, but this is often not the case. Recovery times measured after slower pacing rates are frequently longer than those measured after faster pacing rates. This phenomenon — longer recovery times after slower overdrive suppression — is attributed to the conduction properties of the SA node itself. If conduction within the perinodal cells (cells that surround the pacemaker cells) is abnormal, then SA nodal “entrance block” can occur, wherein some of the paced impulses are blocked from reaching the pacemaker cells. Faster pacing rates can thus actually result in fewer impulses reaching the SA nodal pacemaker cells themselves, and hence in less effective overdrive suppression, than slower pacing rates. This is why a wide range of pacing rates, instead of just the more rapid pacing rates, are used when measuring SNRT. (Assessing the conduction properties of the SA node is discussed below.) In any case, determining the SNRT is easy enough; deciding whether that SNRT is normal or abnormal is a little more problematic. One difﬁculty is that overdrive suppression of the SA node, being a normal phenomenon, occurs in everybody. Unfortunately, there is wide variation in SNRTs among apparently normal individuals as well as considerable overlap in measured SNRTs between patients with apparently normal and clearly abnormal SA nodes.

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Deciding on the upper normal values for the SNRT, then, is not dictated by nature, but by electrophysiologists. “Normal” values vary from laboratory to laboratory, depending on whether electrophysiologists want their measurements to err on the side of sensitivity (in which case a lower value would be used) or speciﬁcity (in which case a higher value would be used). A conservative upper limit of “normal” for the SNRT, above which most experts would agree that SA nodal dysfunction is present, is 1500 msec. Another difﬁculty in interpreting SNRTs is the fact that the SNRT is related to the underlying heart rate (or the basic cycle length, BCL) such that at slower underlying heart rates, a longer recovery time is normally seen. An SNRT that is abnormal at a shorter BCL could be normal at a longer BCL. To account for this relationship between SNRT and BCL, electrophysiologists have created two indices, one or both of which are now measured routinely during electrophysiology studies. The ﬁrst is the corrected sinus node recovery time (CSNRT), which is calculated simply by subtracting the patient’s BCL from the SNRT. Thus: CSNRT = SNRT − BCL By convention, the upper limit of “normal” for the CSNRT is 525 msec. In other words, the SNRT should be no more than 525 msec longer than the BCL. The second index commonly used is the ratio of SNRT to the BCL (SNRT/BCL × 100%). A ratio greater than 160% is usually considered abnormal. Figure 5.1 demonstrates a normal SNRT. Here, the patient’s BCL is 800 msec and the initial recovery interval is 1260 msec. Thus, the SNRT is 1260 msec, the CSNRT (SNRT — BCL) is 460 msec, and the ratio of SNRT to the BCL is 158%. These values are all within normal limits. An abnormal SNRT is demonstrated in Figure 5.2. The BCL in this example is also 800 msec. The longest recovery interval (and thus the SNRT) is 2200 msec. The CSNRT is 1400 msec, and the ratio of SNRT to the BCL is 275%. All of these values are abnormal. These two examples are straightforward in that all the SNRT measures — the SNRT itself, the CSNRT, and the ratio — are either normal (Figure 5.1) or abnormal (Figure 5.2). Not uncommonly, there will be divergence among these three measures. In such cases, the electrophysiologist must use his or her clinical judgment in interpreting the test. Given the relatively arbitrary nature of determining normal from abnormal SNRT values in the ﬁrst place, this circumstance should not add appreciably to one’s level of discomfort. Indeed, once you resort to

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the electrophysiology study for determining whether a patient’s SA node is normal or not, you are already signing up for a certain amount of arbitrariness. Sinoatrial conduction time (SACT)

The sinoatrial conduction time (SACT) test is meant to assess how well the SA node is able to conduct the electrical impulses it produces out to surrounding atrial tissue. The idea that the SA node might not always allow generated impulses to reach the atria came from the observation of SA nodal exit block (see Figure 5.3.) In exit block, a sudden sinus pause occurs with a duration that is exactly twice the normal sinus cycle length, suggesting that an impulse was indeed generated at the right time, but that it failed to conduct out of the SA node. Occasional episodes of exit block are relatively common in patients with SA nodal dysfunction. (SA nodal exit block is analogous to the entrance block we discussed in the discussion of SNRTs, and reﬂects the same physiology.) To understand how such an exit block might occur and how the SACT is measured, it is helpful to visualize the SA node as a small patch of pacemaker cells surrounded by a rim of specialized perinodal tissue that has electrophysiologic characteristics similar to those of the AV node (Figure 5.4). To exit from the SA node, a generated impulse must pass through this rim of perinodal tissue; if conduction is abnormal, exit block may occur. The SACT is a measure of the time it takes an impulse originating in the SA node to travel through the perinodal tissue and into the atria. Prolonged SACTs are thought to indicate abnormal conduction through this tissue, and thus a propensity for SA nodal exit block. To measure SACT, an electrode catheter is placed in the high right atrium near the SA node and atrial pacing is performed to depolarize and thus reset the SA node. The subsequent return interval (i.e., the time from the last paced atrial depolarization to the ﬁrst spontaneous SA

Fig. 5.3 SA nodal exit block. This rhythm strip illustrates SA nodal exit block. Note the sudden sinus pause with a duration that is almost exactly twice the normal sinus cycle length. Presumably, the SA nodal pacemaker cells ﬁred at the appropriate time (indicated by the asterisk), but the impulse was blocked from exiting the SA node thanks to abnormal perinodal conduction. Patients with SA nodal dysfunction commonly display occasional episodes of exit block. These patients usually also have abnormal SACT measurements (see text).

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Fig. 5.4 Measurement of sinoatrial conduction time (SACT). (A) The SA node consists of a patch of pacemaker cells surrounded by a rim of perinodal tissue, which conducts electrical impulses slowly (similar to the AV node). To measure SACT, an electrode catheter is positioned near the SA node and a premature impulse is delivered. The SACT can be deduced by measuring the interval from the premature paced impulse to the next spontaneous impulse (i.e., the return cycle). This return cycle consists of the conduction time into the SA node (B), the normal SA nodal depolarization time (i.e., the basic cycle length [BCL]), (C), and the conduction time out of the SA node (D). (E) illustrates the resultant right atrial electrogram. The SACT is half the difference between the return cycle and the BCL.

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nodal depolarization, as measured from the high right atrial electrode catheter) is assumed to reﬂect the sum of the time it takes for the paced impulse to penetrate into the SA node (at which time it resets the SA node), plus the basic sinus cycle length, plus the time it takes for the subsequent spontaneous beat to penetrate out of the SA node. Assuming that the times of penetration into and out of the SA node are equivalent, then: Return interval = BCL + 2 SACT Because the BCL is known and the return interval can be measured, the SACT can be calculated. In Figure 5.5, the basic cycle length is 800 msec. The paced beat (A2) is assumed to penetrate and reset the SA node, and the return interval is 900 msec. From this formula, 900 msec = 800 msec + 2 SACT. The SACT is thus 50 msec. A normal SACT is considered to be approximately 50 to 125 msec. Two methods have been developed for measuring SACT. In the Narula method, short trains of slow atrial pacing are used, barely faster than the basic sinus rate. A rate just faster than the basic sinus rate is used to minimize any overdrive suppression. (Inducing overdrive suppression would invalidate the SACT calculation, since the SA node would no longer be discharging at its BCL.) In the Strauss method, a series of single premature atrial impulses are used, to guarantee that no overdrive suppression will occur. The principles of both methods, however, are as described above. Whichever method is used to measure SACT, the main limitation of this test is that many patients with SA nodal dysfunction have mod-

Fig. 5.5 Measurement of sinoatrial conduction time (SACT, Strauss method). One surface ECG lead and a right artial (RA) electrogram are shown. Measurements are made from the RA electrogram. A single premature atrial impulse is delivered (A2) at a coupling interval of 780 msec, slightly faster than the basic cycle length (BCL) of 800 msec. The return interval (A2–A3) is 900 msec, which is the BCL + 2 SACT. The SACT is thus 50 msec.

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estly irregular BCLs, which can introduce considerable error into the SACT calculation. Intrinsic heart rate (IHR)

As previously mentioned, the SA node is richly innervated by both sympathetic and parasympathetic ﬁbers. Occasionally, it can therefore be difﬁcult to determine whether suspected SA nodal dysfunction is actually intrinsic to the SA node, or whether it may be due to abnormal autonomic tone. In such cases it can be helpful to measure the intrinsic heart rate (IHR). The IHR is assessed by administering drugs to block both branches of the autonomic nervous system, then measuring the resultant heart rate. Classically, autonomic blockade is accomplished by giving both propranolol (0.2 mg/kg) and atropine (0.04 mg/kg). According to the formula devised by Jose, after autonomic blockade the normal IHR = 118.1 − (0.57 × age). Patients presenting with sinus bradycardia, but who turn out to have normal IHRs, are considered to have normal intrinsic SA nodal function; their bradycardia is apparently due to autonomic inﬂuences. Patients with bradycardia and depressed IHRs are considered to have intrinsic SA nodal dysfunction. Alternately, patients with inappropriate sinus tachycardia (see below) often have substantially elevated IHRs. In clinical practice, it is rarely necessary to measure IHR in order to document intrinsic SA nodal disease. An exercise test, for instance, is a much simpler way to accomplish parasympathetic withdrawal in a patient presenting with sinus bradycardia, and a blunted heart rate response to exercise (in the absence of drugs that cause bradycardia, such as β-blockers and calcium blockers) usually clinches the diagnosis of intrinsic SA nodal dysfunction. Interpreting SA nodal tests: When to carry out electrophysiologic testing

When assessing patients for SA nodal dysfunction, several simple points bear keeping in mind. First, SA nodal dysfunction is generally not a lethal condition, and therapy is necessary only to the extent that it produces symptoms. Second, the best way to diagnose SA nodal dysfunction is to see it occurring spontaneously, because the speciﬁcity of such an observation is 100%. Thus, cardiac monitoring (and not electrophysiologic testing) is the study of choice in assessing SA nodal dysfunction. Third, since the electrophysiology study can help to determine only whether SA nodal dysfunction is present (and not whether it causes

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symptoms), once unexplained sinus bradyarrhythmias are already known to occur, there is generally no reason to consider electrophysiologic testing. Fourth, while the electrophysiology study offers methods for evaluating both the automaticity (SNRT) and conductive properties (SACT) of the SA node, the speciﬁcities and sensitivities of these tests as usually applied are only approximately 70%. With these points in mind, we can conﬁdently state the following guidelines in assessing SA nodal disease: 1 Asymptomatic sinus bradyarrhythmias need no evaluation or treatment. 2 Asymptomatic abnormal SNRTs or SACTs need no treatment. 3 Symptomatic sinus bradyarrhythmias should be treated with pacing, unless they are due to medications or to some other reversible cause. 4 The only inarguable indication for performing electrophysiology studies to assess SA nodal function is to evaluate patients who present with episodic symptoms suggestive of bradyarrhythmias (especially syncope), and for whom no signiﬁcant bradycardia is documented during cardiac monitoring. Inappropriate sinus tachycardia (IST)

Patients with inappropriate sinus tachycardia (IST) have sinus rates that are abnormally high at rest (usually around 100 beats/min; though during sleep the rates may drop to the mid-80s) and that invariably increase rapidly with minimal exertion. They have no identiﬁable reason for secondary sinus tachycardia, such as anemia, infection, hyperthyroidism, pheochromocytoma, substance abuse or cardiopulmonary disease. Their sinus tachycardia is therefore “inappropriate”. While IST can occur in anybody, the typical sufferer is a woman in her 20s or 30s who has been having symptoms for months to years. Prior to the onset of IST, which often follows a viral illness or physical trauma, most of these patients will have been in excellent health, both physically and emotionally. In addition to the most common symptoms of palpitations, fatigue and especially exercise intolerance, IST can also be associated with a host of other symptoms, including orthostatic hypotension, blurred vision, dizziness, tingling, gastrointestinal disturbances, shortness of breath, and sweating. Symptoms can be quite severe, sometimes to the point of being disabling. All these symptoms occur with a paucity of physical ﬁndings or laboratory abnormalities. The only consistent ﬁnding is tachycardia. IST has been a recognized clinical condition only since 1979, and while electrophysiologists by now are very familiar with it, many doctors remain blissfully unaware that it exists. By the time sufferer of

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IST gets to an electrophysiologist, if she’s lucky enough to be referred, she will have been told by at least one doctor that she’s crazy (or, more politely, “anxious”). If the IST itself isn’t enough to make her crazy, then being told it’s all “in her head” may be: By the time she sees an electrophysiologist, anxiety often is indeed an issue. What causes IST?

The cause is unknown. The main question regarding etiology is whether IST is a primary disorder of the SA node, or whether it is instead one of a class of disorders known as the dysautonomias. Electrophysiologists tend to favor the former, but the latter may be more correct. Is IST a primary SA nodal disorder? Several lines of evidence point to IST being a primary SA nodal disorder. First, as we have seen, the intrinsic heart rate in patients with IST tends to be elevated, suggesting that even in the absence of autonomic inﬂuence the SA node displays enhanced automaticity. Second, patients with IST tend to have an abnormally enhanced heart rate response to epinephrine, similar to their exercise response. And third, at least some evidence exists that the SA node in patients with IST is structurally abnormal. It is important to know whether IST is a primary SA nodal disorder because if it is, then ablation of the SA node ought to cure the condition. Accordingly, electrophysiologists have tested this theory by performing SA nodal ablations in hundreds of patients with IST. The outcome is very interesting. The immediate response is usually quite favorable — over 90% of patients no longer have IST immediately after SA nodal ablation. Unfortunately, in about 80% of patients who have such “successful” ablations, the IST recurs within six to nine months. Repeat electrophysiologic testing usually shows regeneration of SA nodal function, complete with its IST-like behavior, though this regenerated SA nodal activity is often found inferior to the original site of ablation, along the crista terminalis. And repeated ablations usually yield the same results — early success and late failure. Thus, something — this “something” being external to the SA node itself — appears to be stimulating regeneration of SA nodal function after ablation. This is the primary piece of evidence against the “primary SA nodal disorder” hypothesis. Is IST a form of dysautonomia? Back in the 19th century, there used to be a condition called “neurasthenia”. Young women (the beautiful but delicate ones, according to the

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romance novels of the time) would ﬁnd themselves suddenly unable to function due to a host of inexplicable symptoms, often including fatigue, weakness, strange pains, dizziness, and passing out. Doctors would not ﬁnd anything to explain these symptoms, so they were attributed to a “weak nervous system”, or neurasthenia. Victims were often conﬁned to their beds, where they would either recover or, eventually (and tragically) die. And while nobody knew what caused this condition, everyone — doctors and laymen alike — took it seriously; the condition and its sufferers were treated with great respect. Today’s doctors shake their heads in wonder at the notion of such a condition, and tend to put neurasthenia in the same bucket as the witchcraft hysteria of a few centuries earlier. But patients who would have been called neurasthenics 150 years ago are still around; they’re just given different labels. These labels include chronic fatigue syndrome (CFS), vasovagal or neurocardiogenic syncope, panic attacks, anxiety, irritable bowel syndrome (IBS), postural orthostatic tachycardia syndrome (POTS), ﬁbromyalgia — and, quite possibly, IST. While most doctors still tend to think of these various syndromes as stand-alone conditions, they are all part of a general class of conditions called the dysautonomias. In dysautonomia the autonomic nervous system loses its normal balance, and at various times the parasympathetic or sympathetic systems inappropriately predominate. Symptoms can include frequent, vague but disturbing aches and pains, faintness or frank syncope, fatigue and inertia, severe anxiety attacks, sinus tachycardia, hypotension, poor exercise tolerance, gastrointestinal disturbances, sweating, dizziness, blurred vision, numbness and tingling, anxiety and (quite understandably) depression. Sufferers of dysautonomia can experience all these symptoms or just a few of them. They can experience one cluster of symptoms at one time — and another at other times. And since people with dysautonomia are usually normal in every other way, a physical exam most often does not reveal any abnormalities. Patients are often labeled hysterical and are accorded little of the respect they received during the 19th century. (Fortunately, doctors no longer prescribe bed rest, so the risk of mortality is now very low.) When patients do get an actual diagnosis, the one they receive does often depend on their recently dominant symptoms and on which specialist they are referred to. What causes dysautonomia? The dysautonomias do not have a single cause. Some patients inherit the propensity to develop dysautonomia syndromes, and variations of dysautonomia often run in families. Viral illnesses can trigger a dysautonomia syndrome. So can exposure to

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chemicals. (Gulf War Syndrome is, in effect, dysautonomia — low blood pressure, tachycardia, fatigue and other symptoms — that, government denials aside, appears to have been triggered by exposure to toxins.) Dysautonomia can result after various types of trauma, especially trauma to the head and chest. (It has been reported to occur for example after breast implant surgery.) Dysautonomias caused by viral infections, toxic exposures, or trauma often have a rather sudden onset. CFS, for instance, most classically begins following a typical viral-like illness (sore throat, fever, muscle aches, and so on), but any of the dysautonomia syndromes can have a similar onset. Is IST one of the dysautonomias? Obviously we do not know for sure, but it certainly shares many of the characteristics of dysautonomia, including that its onset is frequently preceded by a viral illness or trauma; that the patient proﬁle is typical; and that “extra” symptoms frequently occur which are consistent with other forms of dysautonomia. (Indeed, many IST patients might have been labeled as suffering from IBS, POTS or CFS if they had seen someone other than an electrophysiologist.) Further, the fact that something stimulates the successfully ablated SA nodes to regenerate in IST patients suggests a more systemic problem than intrinsic SA nodal disease. And ﬁnally, electrophysiologists have noted that symptoms consistent with dysautonomia often persist even after successful SA nodal ablation (i.e., during the period of time that normal heart rates have been restored). Treatment of IST

If SA nodal ablation offered permanent relief from symptoms, then ablation would quickly become the treatment of choice for many IST sufferers. Unfortunately, however, this is not the case. The mainstay of therapy for IST therefore remains β blockers, calcium blockers, and type Ic antiarrhythmic agents — drugs that suppress SA nodal function — most often in combination. Frequently, with patience and longterm trial-and-error adjustments in medications, the symptoms of IST can be reduced to a tolerable level. Some patients report improvement in symptoms with long-term aerobic training (admittedly difﬁcult to accomplish in patients with profound exercise intolerance); others report improvement from biofeedback techniques, meditation, and other similar practices known to alter autonomic tone. In patients who remain largely disabled from symptoms of IST despite noninvasive efforts at control, SA nodal ablation should be strongly considered despite its drawbacks. Finally, simply waiting may be an option for some patients. The natural history of this disorder has not been well documented, but it

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seems likely that IST tends to improve over time in most individuals. “Doing nothing” may not be an option for patients who are severely symptomatic, but many patients with IST can tolerate their symptoms once they are assured that they do not have a life-threatening cardiac disorder, once they are told that the problem is likely to improve on its own eventually, and once they are enlightened as to the other treatment options.

Evaluation of AV conduction disorders AV conduction disorders are the second major cause of bradyarrhythmias. As with SA nodal disease, the clinician’s chief concern with AV conduction disease is deciding whether the affected patient should receive a pacemaker. This decision is based on three essential pieces of data: Whether the conduction disorder is producing symptoms, the site of the conduction disorder, and the degree of conduction block. Once again, thanks to what has been learned in the electrophysiology laboratory, we usually do not need to perform invasive testing to make this decision. Symptoms of AV conduction disorders

The symptoms that occur with AV conduction disease are the same as those that occur with any bradyarrhythmia: Lightheadedness, dizziness, presyncope, or syncope. Whatever the site or degree of block, AV block that produces any of these symptoms needs to be treated. Often, however, especially with ﬁrst- or second-degree block, AV conduction disturbances are totally asymptomatic. The site of the conduction disorder

Determining the site of the conduction disturbance is important for a simple reason: Block that occurs in the AV node (proximal block) is usually benign, whereas block that occurs in the His-Purkinje system (distal block) is potentially lethal. AV nodal block

Conduction disturbances in the AV node most often have acute, transient, and reversible causes. Ischemia or infarction involving the right coronary artery (which gives off the AV nodal artery in 90% of patients) can cause AV nodal block. Thus, heart block following an inferior myocardial infarction is usually localized to the AV node, and normal AV conduction almost always recovers (though block can persist for days or even weeks.) Acute rheumatic fever and other cardiac

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inﬂammatory conditions can also produce transient AV nodal block. While drugs that affect AV nodal function — mainly digoxin, β blockers and calcium blockers — may produce ﬁrst-degree AV block, higher degrees of drug-induced AV nodal block suggest underlying intrinsic AV nodal dysfunction. Complete heart block localized to the AV node is usually accompanied by the emergence of a relatively reliable escape pacemaker, located just distally to the AV node. This “high junctional” escape rhythm often yields a baseline heart rate of 40 to 55 beats/min, and responds at least moderately well to increases in sympathetic tone. Congenital complete heart block, which is usually localized to the AV node, illustrates the typical, relatively benign character of AV nodal block. Since AV nodal block is usually reversible, it can frequently be managed simply by dealing with the underlying cause; although sometimes temporary pacing support is required in the meantime. His-Purkinje block

In stark contrast to AV nodal block, block occurring distally to the AV node is potentially life-threatening. The potential lethal effect of distal heart block can largely be attributed to the unreliable, unstable, and slow escape pacemakers that tend to accompany this condition. These distal escape pacemakers usually discharge irregularly, 20 to 40 times per minute, and are prone to fail altogether. Thus, syncope, hemodynamic collapse, and death are much more likely to occur when AV block is located in the His-Purkinje system. Furthermore, distal AV block tends to be chronic and progressive in nature, instead of transient and reversible. Distal AV block following myocardial infarction is almost always associated with occlusion of the left anterior descending artery, and thus with anterior myocardial infarctions. His-Purkinje block can also be seen with inﬂammatory and inﬁltrative cardiac disease, with myocardial ﬁbrosis, and in association with aortic valve and mitral valve calciﬁcation. The degree of AV block First degree AV block

In ﬁrst-degree AV block, all atrial impulses are transmitted to the ventricles, but with prolonged conduction times (Figure 5.6). First-degree block is diagnosed from the ECG; all P waves are conducted, but the PR interval is prolonged (usually to between 0.20 and 0.40 seconds, but sometimes much longer.) In most patients with ﬁrst degree AV block, slow conduction is localized to the AV node; slow conduction in the His-

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Fig. 5.6 First-degree AV block. The PR interval in this ﬁgure is approximately 380 msec.

Purkinje system can, however, occasionally cause ﬁrst-degree block. First-degree AV block usually causes no symptoms. Second degree AV block: Mobitz classiﬁcation

In second-degree AV block, intermittent AV block is seen; on the ECG, some P waves are followed by QRS complexes and others are not. Symptoms depend largely on the resultant ventricular rate. When second-degree AV block is observed, one should attempt to classify the block as either Mobitz type I (also called Wenckebach block), or Mobitz type II. The Mobitz classiﬁcation helps to localize the site of the second-degree AV block. In Mobitz type I block, there is a gradual prolongation of the PR interval in the conducted beats immediately preceding a blocked beat (Figure 5.7). The site of Mobitz type I block is usually (but not always) localized to the AV node. (Note that Figure 5.7 shows the unusual case in which Mobitz type I block is due to distal conducting disease.) In Mobitz type II block, the blocked beat occurs suddenly, without any lengthening of the PR intervals in the conducted beats preceding the dropped beat (Figure 5.8). Mobitz type II block always indicates distal block. When differentiating Mobitz I from Mobitz II block, a common mistake is to only compare the PR intervals of successive conducted beats. Sometimes the prolongation in the PR interval from one beat to the next is so subtle that it can be easily missed, in which case Mobitz II block may be mistakenly declared. The best way to tell that the Mobitz I pattern of PR interval prolongation is occurring is to compare the PR interval of the last conducted beat prior to the dropped beat with the PR interval of the ﬁrst conducted beat after the dropped beat. That is, compare the “longest” conducted PR interval to the “shortest” con-

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Fig. 5.7 Mobitz I AV block. A surface ECG and a His bundle electrogram from a patient with Mobitz I AV block are shown. On the surface ECG, progressive prolongation of the PR interval is seen prior to the nonconducted P wave. Although most instances of Mobitz I AV block are located in the AV node, this example illustrates that Mobitz I block occasionally can be seen with disease in the more distal conducting tissue. As seen in the His bundle electrogram, PR prolongation occurs as a result of gradually slowing conduction beyond the His bundle (i.e., the HV interval prolongs), and when block ﬁnally occurs, it occurs below the His bundle.

Fig. 5.8 Mobitz II AV block. This ﬁgure shows three simultaneous surface ECG leads. The nonconducted P wave occurs suddenly, without progressive prolongation in the PR interval. Mobitz II block always indicates distal conducting system disease.

ducted PR interval — a difference between these two PR intervals is almost always easily detectable with Mobitz I block. It is important to realize that the Mobitz classiﬁcation can only be used when you can ﬁnd at least one instance in which two consecutively conducted beats immediately precede a blocked beat. The reason for this limitation is simple — in order for there to be progressive prolongation in the PR interval prior to the dropped beat, at least two consecutively conducted beats must occur. Stating it another way: You cannot use the Mobitz classiﬁcation with 2 : 1 AV block; by deﬁnition, it does not apply (Figure 5.9). Many clinicians make the mistake of automatically classifying 2 : 1 block as Mobitz II, thus misdiagnosing many cases of 2 : 1 AV nodal block as distal block. When 2 : 1 block is present, some means other than Mobitz classiﬁcation must be used to deduce the site of block.

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Fig. 5.9 2 : 1 AV block. Every other P wave in this ﬁgure is nonconducted. The Mobitz classiﬁcation system cannot be applied here.

Third-degree AV block

In third-degree AV block, no atrial impulses are conducted to the ventricles — complete AV block is present (Figure 5.10). Maintaining a ventricular rhythm in the presence of third-degree AV block is totally dependent on subsidiary escape pacemakers. As noted earlier, the reliability of those escape pacemakers is related to the site of block. With AV nodal block, the escape pacemakers tend to be relatively reliable; with distal block, the escape pacemakers tend to be unreliable and slow. Distal third-degree AV block is much more likely to produce symptoms than third-degree block located in the AV node. AV dissociation The presence of AV dissociation can lead to confusion when attempting to discern whether third-degree AV block is present. AV dissociation simply means that the atria and the ventricles are each being controlled by their own independent pacemakers. While AV dissociation is present in all cases of complete heart block, complete heart block is not present in all cases of AV dissociation. Complete heart block is merely one variety of AV dissociation. Figure 5.11 illustrates AV dissociation without complete heart block. Here, normal sinus rhythm is present at a rate of 65 beats/min; but an accelerated junctional pacemaker is also present with a rate of 78 beats/min. Thus, the atrial and ventricular rhythms are functioning independently, i.e., dissociated. Note the fourth P wave in Figure 5.11. This P wave happens to occur at a time when the AV conducting system is no longer refractory from the previous junctional impulse, and it is conducted to the ventricles. Since an appropriately timed atrial complex is conducted, there is no heart block. As a general rule, when the atrial rate is faster than the ventricular rate and no atrial impulses are conducted, complete heart block is present. If the ventricular rate is higher than the atrial rate, AV dissociation without heart block should be suspected.

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Fig. 5.10 Complete heart block with a slow ventricular escape mechanism. Distal heart block is likely in this example.

Fig. 5.11 AV dissociation without complete heart block. In this tracing, the sinus rate is simply slower than the junctional escape rate. The fourth P wave conducts to the ventricles (since the following QRS complex occurs at an PR interval that is narrower than the escape interval of the junctional escape). Thus, not all AV dissociation is complete heart block.

Treatment of AV block

Table 5.1 summarizes the treatment of AV block based on symptoms, the degree of block, and the site of block. In general, determining the presence or absence of symptoms and the degree of AV block is simple. If there is a problem in deciding on therapy, it almost always lies in localizing the site of AV block. Localizing the site of AV block

In most cases, localizing the site of block can be done noninvasively, by evaluating the ECG and performing selected autonomic maneuvers. The ECG can be helpful in several ways. A wide QRS complex indicates the presence of distal conducting system disease and should raise suspicions of infranodal block. In cases of complete heart block, a wide-complex, slow (20 to 40 beats/min) escape pacemaker is a strong indicator of distal AV block; a narrow-complex and more rapid (40 to 55 beats/min) escape rhythm suggests AV nodal block (see Figure 2.3). If second-degree AV block is present, the Mobitz classiﬁcation should be applied (unless the only conduction ratio seen is 2 : 1). Mobitz I block suggests AV nodal disease, whereas Mobitz II block always indicates distal block.

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Table 5.1 Indications for Pacing Based on Site and Degree of AV Block. Should a permanent pacemaker be implanted?

First-degree AV block Second-degree AV block Third-degree AV block

AV nodal block

Distal block

No No† No†

No* Yes Yes

*unless the HV interval is >100 msec; † unless symptomatic bradycardia is present.

Autonomic maneuvers are useful because the AV node has rich autonomic innervation, whereas the distal conducting system does not. Maneuvers that decrease vagal tone or increase sympathetic tone can be expected to improve AV nodal block but not distal block. Maneuvers that increase vagal tone or decrease sympathetic tone will worsen AV nodal block but not distal block. Autonomic maneuvers are especially helpful when either Mobitz type I block or 2 : 1 second-degree AV block is present. In AV nodal block, exercise or atropine administration will improve or resolve the block. In distal block, these same maneuvers will not improve the AV block; and, in fact, the conduction ratio often worsens (e.g., 2 : 1 block may shift to 3 : 1 block; see Figure 5.12). Table 5.2 summarizes noninvasive techniques for localizing the site of AV block. Occasionally, the site of block remains unclear even after a careful noninvasive evaluation. In these instances, the electrophysiology study virtually always resolves the issue. The electrophysiology study in the evaluation of AV conduction disorders

The key to localizing AV conduction disorders in the electrophysiology laboratory is the His bundle electrogram. The recording and interpreting of the His bundle electrogram are described in detail in Chapter 4. In review, the His bundle electrogram consists of three major deﬂections (Figure 5.13). The A deﬂection represents depolarization of atrial tissue proximate to the AV node. The H spike represents the depolarization of the His bundle itself. The V spike represents the depolarization of the ventricular myocardium. The AH interval is therefore an approximation of the conduction time through the AV

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Fig. 5.12 Exercise-induced worsening of AV conduction. (A) shows the resting 12-lead ECG of a patient who had intermittent 2 : 1 AV conduction. With exercise (B), the conduction ratio is markedly worsened, strongly implying distal conducting system disease.

Table 5.2 Noninvasive Differentiation of AV Nodal and Infranodal Block. AV nodal

Infranodal

Exercise/isoproterenol

Improves

Atropine

Improves

Vagal maneuvers β Blockers

Worsens Worsens

Conduction ratio may worsen Conduction ratio may worsen No change No change

Fig. 5.13 A typical His bundle electrogram.

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node (normally 50 to 120 msec), and the HV interval is an approximation of the conduction time through the His-Purkinje system (normally 35 to 55 msec). Thus, the His bundle electrogram reveals the function of all the major components of AV conduction. Overt AV conduction disturbances

In the patient with overt AV conduction disturbances, the His bundle electrogram immediately reveals the site of block. When ﬁrst-degree AV block is localized to the AV node, a prolonged AH interval will be seen (Figure 5.14A), while ﬁrst-degree block below the AV node will produce a prolonged HV interval (Figures 5.14B and 5.15). It should be noted that signiﬁcantly slowed conduction through the His-Purkinje structures can occur without overt ﬁrst-degree AV block. For instance, a lengthening of the HV interval from 50 to 100 msec (a markedly abnormal value) may prolong the PR interval only from 140 to 190 msec (still within the normal range). Occasionally, slowed conduction within the His bundle itself can be observed. The normal conduction time through the His bundle (measured by the duration of the H spike on the His bundle electrogram) is less than 25 msec — a longer H spike duration reﬂects His bundle conduction delay. Sometimes, a His bundle conduction delay is sufﬁciently severe to produce an actual splitting of the His deﬂection (Figure 5.16).

Fig. 5.14 His bundle electrogram patterns seen with ﬁrst-degree AV block. (A) Prolonged conduction in the AV node (the AH interval is prolonged). (B) Prolonged conduction below the AV node (the HV interval is prolonged).

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Fig. 5.15 Distal ﬁrst-degree AV block. A surface ECG lead and the His bundle electrogram are shown from a patient with ﬁrst-degree AV block. The conduction delay can be seen to occur in the distal structures because the AH interval is normal and the HV interval is prolonged.

Fig. 5.16 Split His. Conduction disease within the His bundle itself is present because the His bundle is split into two discrete components. A split His potential indicates signiﬁcant distal conducting system disease.

While there is no general agreement on whether to treat patients with asymptomatic prolongations in the HV interval, most physicians agree that a permanent pacemaker is indicated if the HV interval is very prolonged (i.e., greater than 100 msec), or if a split His is present. With second-degree AV block of the Mobitz I type (Figure 5.17), the intracardiac electrogram usually shows a progressive prolongation of the AH interval in the beats immediately prior to the dropped atrial

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Fig. 5.17 Typical Mobitz I AV block. A surface ECG lead and the His bundle electrogram are shown. Note the progressive prolongation of the AH interval (and the PR interval) prior to the nonconducted P wave. The blocked beat occurs when the impulse fails to exit the AV node (the A complex is not followed by an H spike in the blocked beat). This is much more typical for Mobitz I AV block than the example shown in Fig. 5.7.

impulse (indicating a gradual slowing in conduction through the AV node before the dropped beat). With the dropped beat itself, the A deﬂection is not followed by an H spike, indicating block within the AV node. Again, while Mobitz type I block usually indicates AV nodal block, a Mobitz I pattern is occasionally seen with block in the His-Purkinje system (see Figure 5.7). Mobitz type II block (Figure 5.18) is always located in the HisPurkinje system. Thus, the His bundle electrogram shows a normal AH interval and a stable HV interval in all the conducted beats, but in the dropped beat there is suddenly no ventricular depolarization after the H spike. With third-degree block within the AV node, the A spikes are not followed by H spikes. Further, since the escape pacemaker is usually proximal to the His bundle, escape pacemaker complexes are usually preceded by His potentials (Figure 5.19A). With third-degree block occurring in the His-Purkinje system, the A spike is followed by an H spike, but there is no V spike after the H. The escape ventricular electrogram is not preceded by a His potential, since these escape pacemakers are distal to the His bundle (Figure 5.19B). Inapparent AV conduction disturbances

Patients may present with symptoms compatible with AV conduction disease, but neither the ECG nor monitoring conﬁrms any conduction abnormalities. In such cases the electrophysiology study can be quite helpful.

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Fig. 5.18 Mobitz II AV block. The His bundle electrogram is shown. The beat is dropped after the H spike and has no prior prolongation in either the AH or HV interval.

Fig. 5.19 His bundle electrograms in complete heart block. (A) With block in the AV node, H spikes are seen prior to the escape V complexes, indicating a high junctional escape pacemaker. No H spikes are seen after the blocked A complexes, indicating block in the AV node. (B) With distal AV block, an H spike follows each nonconducted A complex. The distal ventricular escape complexes are not preceded by H spikes.

The goal in electrophysiologic testing is to stress AV conduction by pacing the right atrium, while recording the His electrogram to see what happens. Two primary pacing methods are used, as described in Chapter 4: The extrastimulus technique (in which a single atrial premature stimulus is introduced, after a drive train of stimuli at a ﬁxed cycle length) and incremental pacing. The extrastimulus technique This technique is illustrated in Figures 5.20 through 5.22. Following a drive train of several (usually eight) incrementally paced beats (the S1 beats) at a ﬁxed cycle length (usually 600 msec), a single premature atrial stimulus is introduced (the S2 beat). The coupling interval between the last S1 beat and the S2 beat is initially relatively long (usually 500 msec), but with each subsequent pacing sequence the S1–S2 coupling interval is progressively shortened. The goal is to determine when AV block ﬁrst occurs and where it ﬁrst occurs (i.e., in or distal to the AV node) in response to the S2 impulses.

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Fig. 5.20 The extrastimulus technique, A. In the following series of ﬁgures (5.20 through 5.22) a typical response to the atrial extrastimulus technique is shown. Three surface ECG leads, one right atrial electrogram, three His bundle electrograms, and one right ventricular electrogram are shown. In this ﬁgure, the S1–S2 coupling interval of 480 msec is followed by a minimal prolongation of the AH interval.

The normal sequence of events is shown in Figures 5.20 through 5.22. The AH interval and HV interval measured during the S1 drive train are considered to represent the baseline AV node and His-Purkinje conduction times. Any prolongations in AH and HV intervals observed with the S2 beat then reﬂect slowed conduction in response to premature impulses. Initially, the S2 beat is conducted normally, with little or no delay in either the AH or HV intervals (see Figure 5.20). As the S1–S2 coupling interval becomes gradually shorter, the relative refractory period (RRP) of the AV node is reached (i.e., at this point conduction through the AV node becomes prolonged — see Chapter 4 for a review of the deﬁnitions of relative, effective, and functional refractory periods). Thus, the AH interval becomes longer (see Figure 5.21). With progressively shorter S1–S2 intervals, the resultant AH interval becomes even longer, until ﬁnally the S2 beat is so early that block occurs in the AV node (see Figure 5.22). The coupling interval that produces block in the AV node is the effective refractory period (ERP) of the AV node. By measuring the H1–H2 intervals that result with each pacing sequence, the functional refractory period (FRP) of the AV node can be determined (the FRP of the AV node is the shortest H1–H2 interval attained). The His-Purkinje ERP is usually signiﬁcantly shorter than the AV nodal

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Fig. 5.21 The extrastimulus technique, B. With further shortening of the S1–S2 coupling interval (to 440 msec), progressive prolongation in the AH interval is seen (compare this A2–H2 interval to the A2–H2 interval in Fig. 5.20).

Fig. 5.22 The extrastimulus technique, C. With an S1–S2 coupling interval of 320 msec, the S2 stimulus is blocked in the AV node (the A2 complex is not followed by an H spike).

FRP, so that the His-Purkinje structures are usually “protected” by the conduction delays in the AV node. Thus, block in the His-Purkinje system is seldom seen during the extrastimulus technique in normal patients. Figure 5.23 shows an abnormally prolonged AV nodal ERP. At a coupling interval of 480 msec, the S2 impulse is blocked in the AV node. The

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Fig. 5.23 Abnormal AV nodal function brought out by the extrastimulus technique. The same leads are depicted as in Figs. 5.20 through 5.22. With an S1–S2 coupling interval of 480 msec, block occurs in the AV node.

signiﬁcance of this ﬁnding would depend largely on whether the patient showed evidence of symptomatic bradyarrhythmias. If so, and if the AV nodal dysfunction is intrinsic (i.e., not reversible), pacing might be considered. Note that in this example, it would be difﬁcult to diagnose concomitant His-Purkinje disease because the long ERP (and thus the long FRP) of the AV node prevent us from evaluating the effect of early impulses on the more distal structures. To evaluate the His-Purkinje system in such a patient, it would be necessary to attempt to improve AV nodal function by administering atropine or isoproterenol. An example of abnormal His-Purkinje function is shown in Figure 5.24. At an S1–S2 interval of 460 msec, the impulse is conducted normally to the His bundle through the AV node (we know this from the normal AH interval), but infranodal block is present because the impulse is not conducted to the ventricles (i.e., the H spike is not followed by a V spike). Block in the His-Purkinje system at an H1–H2 interval of greater than 400 msec indicates signiﬁcant distal conducting system disease. Incremental pacing With this technique (illustrated in Figures 5.25 through 5.27), long sequences of right atrial pacing are introduced while observing the behavior of the AV node and the His-Purkinje system. A pacing rate

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Fig. 5.24 Abnormal His-Purkinje function brought out by the extrastimulus technique. With an S1–S2 coupling interval of 460 msec, block occurs below the His bundle (the H spike is not followed by a V complex). A surface ECG lead and two His bundle electrograms are shown.

slightly faster than the underlying sinus rate is used initially. The pacing rate is gradually increased with each subsequent pacing sequence. The normal response to incremental pacing is shown in Figures 5.25 through 5.27. At progressively faster atrial pacing rates, the AH interval gradually increases until the refractory period of the AV node is reached, at which time second-degree AV block occurs, typically in a Mobitz I pattern. In this case, the AH interval gradually prolongs from 110 msec at a paced cycle length of 600 msec (Figure 5.25) to 160 msec at a cycle length of 450 msec (Figure 5.26). Finally, in Figure 5.27, at a cycle length of 400 msec, Mobitz I second-degree AV block is seen (note the gradually increasing AH intervals prior to the dropped beat). The atrial pacing

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Fig. 5.25 Incremental atrial pacing, A. Figures 5.25 through 5.27 show the normal response to incremental atrial pacing. All three ﬁgures display three surface ECG leads followed by one right atrial electrogram, two His bundle electrograms, two coronary sinus electrograms, and one right ventricular electrogram. In this ﬁgure, incremental pacing from the high right atrium at a cycle length of 600 msec results in normal AV conduction (as shown in the labeled His bundle electrogram).

rate at which Mobitz type I block occurs is called the Wenckebach cycle length. Normally, the Wenckebach cycle length is less than or equal to 450 msec. During incremental atrial pacing, the Wenckebach cycle length is normally encountered before any prolongation of the HV interval is seen. Lengthening of the HV interval, or block in the His bundle, occurring at a paced cycle length of greater than or equal to 400 msec indicates an abnormal distal conducting system. An example of distal block is shown in Figure 5.28. At a cycle length of 460 msec, intermittent seconddegree AV block is seen. The His electrogram reveals a constant AH interval, with intermittent block occurring in the His-Purkinje system (in dropped beats, H spikes are not followed by V spikes). Once again, if distal conducting system disease is suspected but the AV nodal refractory periods are too long to allow the His-Purkinje system to be fully evaluated, autonomic maneuvers should be considered to reduce the refractoriness of the AV node and to permit further testing of the infranodal conducting system.

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Fig. 5.26 Incremental atrial pacing, B. At a faster incrementally paced cycle length (450 msec), prolongation in the AH interval (compared to Fig. 5.25) is apparent. All atrial impulses, however, are conducted.

Fig. 5.27 Incremental atrial pacing, C. At a paced cycle length of 400 msec, Mobitz I conduction occurs. Note the progressive prolongation in the AH intervals in the beats preceding the nonconducted P wave. Thus, the Wenckebach cycle length is 400 msec (a normal value).

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Fig. 5.28 Distal AV block during incremental atrial pacing. In this ﬁgure, during incremental atrial pacing, 2 : 1 AV block occurs. The His bundle electrogram shows that the block is in the distal conducting system — the AH interval is constant, and there is an H spike in the nonconducted beats.

Bundle branch block As we saw in Chapter 1, the His bundle divides into two main branches — the right and left bundle branches. Thus, electrical impulses exiting the AV conduction system are rapidly transmitted through the right and left bundle branches, then through successive branches of Purkinje ﬁbers, and ﬁnally to the right and left ventricular myocardium. The bundle branches and Purkinje system distribute the electrical impulse across the ventricular myocardium in such a way as to optimally coordinate the contraction of both ventricles. The bundle branches and Purkinje ﬁbers are subject to the same sorts of disorders as the rest of the cardiac conducting system. When there is a general slowing of conduction in or distal to the bundle branches, the distribution of the electrical impulse to the ventricular myocardium is delayed, and an intraventricular conduction delay (IVCD) is said to be present. An IVCD is manifested on the surface ECG by a wide QRS complex. Delayed or blocked conduction is commonly limited speciﬁcally to either the right or the left bundle branch, conditions referred to as right or left bundle branch block. Thus, right bundle branch block (RBBB) and left bundle branch block (LBBB) are speciﬁc varieties of IVCD. Right bundle branch block (RBBB)

RBBB is a relatively common ECG ﬁnding that generally carries little prognostic signiﬁcance. The incidence of RBBB gradually increases with age, from less than 1% in 50-year-olds to approximately 10% in octogenarians. Most younger patients with RBBB have no underlying heart disease.

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The right bundle branch remains a relatively discrete structure for a few centimeters after splitting off from the His bundle, and for most of its course it is located just beneath the endocardial surface, where it is subject to stretch and trauma from conditions affecting the right ventricle. Thus, RBBB is common in conditions causing pulmonary hyper tension, or right ventricular hypertrophy, inﬂammation, or infarction. RBBB can appear quite abruptly with sudden elevations in right-sided cardiac pressures, as in pulmonary embolism. RBBB can also occur during right heart catheter insertions due to localized trauma to the right bundle branch — this latter form of RBBB, which is seen in roughly 5% of right heart catheterizations, is usually transient. The prognosis of patients with RBBB is dictated not by the RBBB itself, but almost entirely by the type and severity of any underlying heart disease. If there is no underlying heart disease — that is, if RBBB is an isolated ﬁnding in an otherwise normal patient — the long-term prognosis appears virtually normal. As long as the left bundle branch functions normally, patients with RBBB do not appear to suffer from clinically signiﬁcant ventricular dyssynchrony; that is, left ventricular contractions remain coordinated and efﬁcient. The presence of RBBB alone is never an indication for a permanent pacemaker. Left bundle branch block (LBBB)

LBBB, while not uncommon, is seen less frequently than RBBB. The incidence of LBBB is less than 0.5% in 50-year-olds, but increases to 5– 6% by age 80. (The age-related increase in frequency seen with both varieties of bundle branch block suggests a degenerative disorder of the conducting system, similar to the process that causes SA nodal and AV conduction abnormalities in the same age group.) Younger patients with LBBB usually have no underlying heart disease, in which case the prognosis is excellent. In older patients, for whom the new onset of LBBB most often indicates the presence of progressive heart disease (most commonly coronary artery disease, cardiomyopathy, or valvular heart disease), LBBB is an independent predictor of mortality. There are at least two reasons why LBBB may indicate a worse prognosis in patients with underlying heart disease. The ﬁrst is related to the fact that the left bundle branch almost immediately divides into three major fascicles after splitting off from the His bundle, and thus quickly becomes a relatively diffuse system. For this reason, the presence of LBBB (in contrast to RBBB) both suggests a diffuse pathological process instead of a localized one, and frequently indicates

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that advanced heart disease is present. And second, the LBBB itself produces disordered left ventricular contraction and in patients with underlying systolic dysfunction can directly worsen cardiac performance. (See Chapter 9, especially Figure 9.1, for an explanation of how LBBB produces ventricular dyssynchrony.) In many cases, patients with LBBB and heart failure can be helped with cardiac resynchronization therapy (CRT) — specialized pacemakers that pace both ventricles simultaneously, thus re-coordinating ventricular contraction. (See Chapter 9 for a detailed discussion of CRT.) The presence of LBBB alone does not constitute an indication for a standard, anti-bradycardia permanent pacemaker. As noted, however, in some clinical circumstances patients will have an indication for CRT pacemakers by virtue of their LBBB. Further, when performing a right heart catheterization in patients with LBBB, provisions for immediate temporary pacing support should be available, since there is a 5% chance of causing transient RBBB (and thus complete heart block) during the procedure. In addition, some patients experiencing block in one of the fascicles of the left bundle branch in combination with RBBB (a condition known as bilateral fascicular block) and a myocardial infarction, have an increased risk of complete heart block and should receive permanent pacemakers.

A brief overview of permanent pacemakers Major indications for pacemakers

In the preceding discussion, we have touched upon the major indications for permanent pacemakers. The following list makes these indications more explicit: 1 Symptomatic sinus bradycardia a. Symptomatic sinus bradycardia at rest. b. Inability to increase the sinus rate appropriately with exercise (i.e., chronotropic incompetence), thus limiting exercise capacity. c. Syncope of unknown origin in patients who are shown to have signiﬁcant SA nodal abnormalities on electrophysiologic testing. 2 AV conduction disease a. Acquired 3rd degree AV block. b. 2nd degree AV block below the AV node. c. 2nd degree AV nodal block if persistent and symptomatic. d. New bilateral fascicular block following an acute myocardial infarction. e. Congenital complete heart block with severe bradycardia, signiﬁcant symptoms, or wide-QRS escape rhythm. f. Markedly prolonged HV interval (>100 msec,) or split His.

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3 Other indications for pacing a. Cardioneurogenic syncope (also known as vasovagal syncope; see Chapter 10), in which there is a severe or persistent component of bradycardia, in patients in whom more conservative therapeutic attempts have failed. b. Syncope of unknown origin in the presence of bilateral fascicular block, where no other cause of syncope can be identiﬁed. c. Bradycardia-induced ventricular tachyarrhythmias. d. Cardiac resynchronization therapy (CRT). CRT is indicated for many patients with signiﬁcant LV dysfunction (ejection fraction less than 0.35) and wide QRS complex (QRS duration more than 120 msec). CRT is discussed in detail in Chapter 9. Pacemaker nomenclature

While in practical terms most pacemakers can be separated into one of two categories — single-chambered or dual-chambered pacemakers — any pacemaker can be programmed to a potentially bewildering array of “modes”. If we view a pacemaker as a tiny computer enclosed within an implantable metal can, the pacing mode can be thought of as the set of instructions — or the software program — that tells the pacemaker how to function under various circumstances. By convention, pacing modes are described by a three-letter code ﬁrst promulgated over 30 years ago. As pacemakers have become more complex over the ensuing decades, various attempts have been made to expand the three-letter code to as many as ﬁve or six letters, but the original three-letter code still tells us most of what we need to know. The ﬁrst letter indicates the chamber or chambers that are paced. “A” indicates the atrium; “V” indicates the ventricle; and “D” (which stands for dual chamber) indicates both atrium and ventricle. The second letter indicates the chamber or chambers in which sensing occurs. Again, “A” indicates the atrium; “V” indicates the ventricle; “D” indicates both atrium and ventricle; and “O” means no sensing is occurring. The third letter indicates how the pacemaker responds to a sensed event. “I” means that a sensed event causes inhibition of the pacing impulse (and resets the timing intervals). “T” stands for a sensed event triggering a pacing impulse. “D”, which is only used in dual-chambered devices, means there is a “dual” (or two kinds of) response — a sensed event can either inhibit or trigger a pacing impulse, depending on circumstances. “O” means that a sensed event neither inhibits nor triggers a pacing impulse — it is “ignored”.

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In addition, a fourth letter is often employed to indicate that rateresponsive pacing is being used. Rate-responsive pacing incorporates a sensor into the pacing system that continually monitors the physiologic needs of the patient. The rate of pacing is thereby adjusted to the physiologic requirements of the patient from moment to moment. The sensors used most commonly in today’s pacemakers monitor either activity or respiratory rate — the more active the patient or the more rapidly they are breathing, the higher the rate of pacing (within a programmed limit). The fourth letter “R” is added to the three-letter code if rate-responsive pacing is active. Common modes of pacing

For practical purposes, only two modes are used with any frequency, the VVI (or AAI) mode for single-chambered pacemakers, and the DDD mode for dual-chambered pacemakers. VVI or AAI pacing

Single-chambered pacemakers function in the VVI mode when the pacing lead is positioned in the ventricle and in the AAI mode when the lead is in the atrium. These pacemakers simply maintain a minimum programmable heart rate. Each timing sequence is initiated either by a paced impulse or a sensed (i.e., intrinsic) impulse. If an intrinsic beat does not occur (i.e., is not sensed) by the end of this timing sequence, a paced impulse is delivered and a new timing sequence is begun. (Thus, a VVI pacemaker paces in the ventricle [V], senses intrinsic beats occurring in the ventricle [V], and a sensed event causes it to inhibit pacing and resets the timing sequence [I]) Essentially then, the doctor programs a minimum heart rate, and whenever the patient’s intrinsic heart rate falls below that value, pacing occurs at the programmed rate; if the intrinsic heart rate is above the programmed rate, pacing is inhibited. An electrogram from a VVI pacemaker is illustrated in Figure 5.29. AAI pacemakers work in exactly the same way, except that the pacing lead is located in the atrium instead of the ventricle. AAI pacing is used exclusively in patients with isolated SA nodal dysfunction; that is, patients who show no evidence of AV conduction disease. For such patients, AAI pacing provides both rate support and AV synchrony and is an excellent choice. AAI pacing is not used commonly in the United States (apparently American doctors are afraid either of occult AV conduction disease or of American lawyers) but is employed quite frequently in many other countries. VVI pacemakers offer perfectly acceptable protection from bradyarrhythmias but do not restore AV synchrony. In general, VVI pacemakers

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Fig. 5.29 VVI pacing. This surface ECG tracing is from a patient with a VVI pacemaker. A VVI pacemaker paces the ventricle at a ﬁxed rate, unless intrinsic ventricular activity is sensed during the pacemaker escape interval. (The pacemaker escape interval is the length of time after a QRS complex during which the pacemaker waits for an intrinsic QRS complex before ﬁring.) The ﬁrst four beats show ventricular pacing. After the fourth paced beat, an intrinsic QRS complex occurs during the pacemaker escape interval. This inhibits the pacemaker from ﬁring and resets the pacemaker escape interval. Two more intrinsic QRS complexes occur, and the pacemaker remains appropriately inhibited.

are used in patients who are felt to need only rare to occasional ventricular pacing support. Practically speaking, almost all single-chambered pacemakers in use today are programmed to rate-responsive modes (i.e., either AAIR or VVIR pacing modes), so the rate of pacing is not ﬁxed but adjusts from minute to minute according to the needs of the patient. Since AAI pacing is used exclusively in patients with SA nodal disease, and thus in patients who are likely to have a blunted heart rate response to exercise, it is difﬁcult to imagine a circumstance in which AAI pacing would be chosen over AAIR pacing. VVIR pacemakers are a good choice for patients with chronic atrial ﬁbrillation. Pacemaker syndrome The major clinical problem inherent in VVI/R pacing is pacemaker syndrome. Pacemaker syndrome arises when intrinsic atrial impulses occur during or just after ventricular pacing, thus causing the atria to contract against closed AV valves, and producing reﬂux of atrial blood through the superior vena cava and pulmonary veins. Symptoms may include headache, dizziness, fatigue, lethargy, neck throbbing, cough, dyspnea, chest “fullness”, and, occasionally, orthostatic hypotension or syncope. Pacemaker syndrome is especially prevalent in patients who have intact

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retrograde conduction, where retrograde impulses stimulate atrial contraction immediately after ventricular pacing. In some series, more than 20% of patients who require frequent VVI pacing display some degree of pacemaker syndrome. Pacemaker syndrome is resolved by changing over to a dual-chambered pacemaker. Patients with chronic atrial ﬁbrillation are not subject to pacemaker syndrome. DDD pacing

Modern dual-chambered pacemakers almost always function in the DDD mode. In DDD pacing, pacing occurs in both the right atrium and the right ventricle (D), senses in both the atrium and the ventricle (D), and a sensed event can either trigger or inhibit a pacing output (D), see Figure 5.30. DDD pacemakers are designed to preserve the normal sequence of AV contraction under a wide range of circumstances and, if the SA node is functioning normally, to allow tracking of the intrinsic sinus rate. Atrial pacing occurs if the intrinsic atrial rate falls below the minimum programmed heart rate. After a paced or sensed atrial event, the pacemaker will wait a certain length of time (i.e., the programmed AV interval) for the ventricle to depolarize. If no intrinsic ventricular activity is detected during that interval, the ventricle is then paced. Most dual-chambered pacemakers used today offer a rate-responsive mode (i.e., the DDDR mode) to allow higher heart rates in response to physiologic needs, even if the SA nodal dysfunction is present. DDDR pacing is ideal for patients with both SA nodal and AV conduction disorders. Mode switching In the past, DDD pacing was often difﬁcult to manage in patients with episodic atrial tachyarrhythmias, since the pacemaker would track the atrial tachycardia and pace the ventricle at inappropriately high rates. Most modern dual-chambered pacemakers now provide a modeswitching feature that largely eliminates this problem. Under mode switching, when an atrial tachyarrhythmia occurs, the pacemaker automatically switches to a non-atrial-tracking mode, most commonly to the VVI (or VVIR) mode. When the atrial arrhythmia terminates, the pacemaker switches back to the DDD (or DDDR) mode. Pacemaker tachycardia The most common clinical problem inherent to DDD pacemakers is pacemaker tachycardia, in which a) a premature ventricular complex causes a retrograde impulse to be transmitted to the atrium; where b) it

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Fig. 5.30 DDD pacing. DDD pacing is designed to maintain AV coordination under most circumstances. DDD pacing can be described largely by considering two escape intervals, the VA interval and the AV interval (both of which are programmable with DDD pacemakers). When a QRS complex occurs (either intrinsic or paced), the VA interval is reset. If no intrinsic atrial or ventricular activity is sensed by the end of the VA interval, an atrial pacing spike is delivered. Once an atrial event occurs (either a paced or intrinsic atrial event), the AV interval is initiated. If no intrinsic ventricular activity occurs during the AV interval, a ventricular pacing spike is delivered at the end of that interval. (A) An intrinsic P–QRS complex occurs during the VA interval, and all pacing is inhibited. (B) No atrial or ventricular activity is sensed during the VA interval, and atrial pacing occurs. During the ensuing AV interval, normal conduction occurs to the ventricle, so ventricular pacing is inhibited. (C) Same as in (B), except that this time conduction to the ventricles does not occur during the AV interval, so the ventricle is paced.

is sensed by the atrial lead and interpreted by the pacemaker as an intrinsic atrial beat; so that c) the pacemaker then triggers a ventricular paced beat; which again d) transmits a retrograde impulse to the atrium — thus establishing a pacemaker-mediated “reentrant tachycardia” (Figure 5.31). In the typical case, pacemaker tachycardia occurs at the maximum programmed pacing rate.

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Fig. 5.31 Pacemaker tachycardia. With DDD pacemakers, the potential for a reentrant tachycardia exists, the pacemaker itself serving as the antegrade limb of the reentrant circuit. Pacemaker tachycardia is most often initiated by a PVC, which conducts retrogradely to the atrium. The atrial electrode of the pacemaker senses the retrograde atrial impulse and initiates the AV escape interval (see Fig. 5.30) of the DDD pacemaker. At the end of the AV interval, a ventricular pacing spike is delivered. If this paced ventricular impulse again conducts retrogradely to the atrium, an incessant tachycardia can result.

A number of methods have been used to control pacemaker tachycardia. • Lengthening the post-ventricular atrial refractory period (PVARP) can essentially “blind” the atrium for a time after a ventricular event, to reduce the odds that a retrograde P wave will be sensed. Unfortunately, increasing the PVARP also reduces the maximum tracking rate the pacemaker will allow. • Reducing the sensitivity of the atrial lead so that SA nodal impulses can still be detected, but retrograde P waves (which often have relatively small amplitudes) cannot. • Many modern pacemakers incorporate a feature that automatically lengthens PVARP for one cycle following a premature ventricular complex, which can inhibit the initiation of pacemaker tachycardia. • Special algorithms, available in some pacemakers, can automatically withhold a single ventricular paced impulse after a certain number of

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beats, whenever the pacemaker is pacing at the maximum tracking rate. This single inhibited ventricular impulse will terminate pacemaker tachycardia. In general, by using one or more of these strategies, pacemaker tachycardia can be managed adequately. CRT pacing

Cardiac resynchronization therapy — also known as biventricular pacing — is done not to provide bradycardia support, but instead to improve left ventricular hemodynamic function in patients with both systolic heart failure and signiﬁcant IVCDs. CRT therapy is discussed in detail in Chapter 9. Deciding which pacemaker to implant

The choice as to which kind of pacemaker to implant — a singlechambered or a dual-chambered pacemaker — is largely an empiric one. Randomized trials designed to detect a signiﬁcant difference in outcomes between these two general types of pacemakers largely have failed to do so. Speciﬁcally, the risk of mortality and stroke is not measurably improved for one type of pacemaker over the other. In general, however, most electrophysiologists feel that maintaining AV synchrony still provides signiﬁcant beneﬁts. Avoiding overt or subtle pacemaker syndrome is one such beneﬁt. Another is that the incidence atrial ﬁbrillation appears be reduced with dual-chambered pacing (quite possibly because the atrial stretching that occurs when the atria contract against closed AV valves may increase the likelihood of atrial ﬁbrillation). Thus, maintaining AV synchrony seems to have real beneﬁts in many patients and should be a major consideration in selecting the appropriate pacemaker for a patient. The other major consideration is maintaining rate-responsiveness, since one’s ability to perform physical activity is strongly dependent on the ability to increase the heart rate appropriately with exercise. Keeping these two major considerations in mind (i.e., maintaining both AV synchrony and rate-responsiveness), the appropriate pacemaker can usually be selected by answering two fairly simple questions (Figure 5.32). The ﬁrst is: “Is there chronic atrial ﬁbrillation?” If so, maintaining AV synchrony becomes moot, and a single-chambered VVIR pacemaker should be used. In virtually all other cases, a dualchambered pacemaker is preferable. The second question is: “Is there SA nodal dysfunction?” If the SA node is known to be normal, then a simple DDD pacemaker can provide

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Fig. 5.32 Decision tree for deciding which type of pacemaker to implant.

both AV coordination and rate responsiveness. On the other hand, if the SA node is either known or suspected to be abnormal, then a dualchambered pacemaker capable of the DDDR mode should be used. Is the electrophysiology study helpful in selecting the right pacemaker? Generally, the electrophysiology study is not helpful in selecting the right pacemaker, but on occasion it can be. If one would like to use a DDD instead of a DDDR pacemaker in a patient with AV block, for instance, ﬁrm evidence of normal SA nodal activity would be helpful, and an electrophysiology study could provide that evidence. There is, however, little advantage at present in choosing a dual-chambered pacemaker that does not provide rate-responsive pacing, as the cost differential between DDD and DDDR pacemakers is now usually quite small. Indeed, almost all currently manufactured dual-chambered pacemakers offer rate-responsive pacing. The other circumstance in which electrophysiologic testing may be helpful is when considering an AAIR pacemaker. (In deference to American electrophysiologists, AAIR pacing is not included in Figure 5.32.) In patients with pure SA nodal disease and normal AV conduction, an AAIR pacemaker will result in both AV synchrony and

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rate responsiveness and would be a very reasonable choice. Unfortunately, at least one-third of patients with SA nodal disease have concomitant AV conduction disease. Thus, electrophysiologic testing should be considered prior to using AAI pacing, in order to rule out subtle conduction abnormalities. Indeed, one advantage of avoiding the AAI mode altogether is that doing so virtually eliminates the need to ever do electrophysiologic testing in deciding which pacemaker to implant.

CHAPTER 6

The Electrophysiology Study in the Evaluation of Supraventricular Tachyarrhythmias

The electrophysiology study has revolutionized our understanding and treatment of supraventricular tachyarrhythmias. The ability to study these arrhythmias accurately has allowed us to classify them precisely according to mechanism, and this reclassiﬁcation has helped greatly to direct appropriate therapy. Correlating ﬁndings from the electrophysiology laboratory with ﬁndings on the surface ECG has allowed clinicians to choose speciﬁc therapy in many patients, even without invasive testing. Further, the electrophysiology study has allowed us to identify effective therapy for patients with complex or difﬁcult forms of supraventricular arrhythmias whose therapy would likely have been unsatisfactory in earlier days. The study of supraventricular tachyarrhythmias is the most challenging and intellectually satisfying type of electrophysiology study. Unlike the studies performed for bradyarrhythmias (the novelty of which soon fades for the budding electrophysiologist), no two studies for supraventricular tachyarrhythmias are exactly alike. When investigating supraventricular tachycardia, unpredicted ﬁ ndings are commonplace. The electrophysiologist must therefore be alert for unexpected results and must be ready to alter the procedural plan to pursue fully those ﬁndings. As opposed to studies performed for ventricular tachyarrhythmias, there is no need to take it on faith during studies for supraventricular tachycardias that the arrhythmias being induced are reentrant. In many patients with supraventricular tachyarrhythmias, the anatomic pathways for the reentrant circuit can be deﬁned with surprising accuracy. In fact, most electrophysiologists starting off in the profession do not truly believe in the reality of reentrant circuits until they perform a few electrophysiology studies in patients with supraventricular tachycardia. In this chapter, we will review the various types of supraventricular tachyarrhythmias and describe how the electrophysiology study helps 103

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to elucidate the mechanisms and most appropriate therapy for these arrhythmias.

General classiﬁcation of supraventricular tachyarrhythmias As described in Chapter 2, most supraventricular tachyarrhythmias are due to either abnormal automaticity or reentry. Automatic supraventricular tachyarrhythmias

Automatic supraventricular tachyarrhythmias are relatively uncommon, except in acutely ill patients. When they do occur, they are usually associated with fairly obvious metabolic disturbances, the most common being myocardial ischemia, acute exacerbations of chronic lung disease, acute alcohol ingestion, and electrolyte disturbances. The arrhythmias usually arise from ectopic automatic foci located somewhere within the atrial myocardium. Characteristically, automatic atrial tachycardias display the typical warm-up phenomenon seen with automatic rhythms (i.e., the rate accelerates after its initiation). The peak rate is usually less than 200 beats/min. There is a discrete P wave before each QRS complex, and the P wave conﬁguration generally differs from the sinus P wave (depending on the location of the automatic focus within the atria). Because the AV node is not necessary for the maintenance of the arrhythmia, AV block is commonly seen during automatic atrial tachycardia; interventions that affect AV conduction may produce block but do not affect the tachycardia itself. Digitalis toxicity often presents as atrial tachycardia with AV block and, while the mechanism is felt to be triggered automaticity, this arrhythmia is clinically indistinguishable from standard automatic atrial tachycardia. Thus, any unexplained atrial tachycardia with block should prompt a search for digitalis toxicity. Multifocal (or chaotic) atrial tachycardia (Figure 6.1) is a form of automatic atrial tachycardia characterized by multiple (usually, at least three) P wave morphologies and irregular PP intervals. It is thought to be due to multiple atrial automatic foci which are ﬁring at differing rates. Multifocal atrial tachycardia is often seen with acute pulmonary disease and may be related to theophylline use. Inappropriate sinus tachycardia (IST) is a unique type of automatic tachycardia originating in the sinus node. Consequently, except for the clinical setting, IST is identical to normal sinus tachycardia. (IST is discussed in detail in Chapter 5 and is mentioned here mainly to point out how it differs from other, more typical forms of automatic tachycardia.)

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Fig. 6.1 Multifocal atrial tachycardia. This is an irregularly irregular rhythm with multiple (but discrete) P wave morphologies. It is thought to be due to multiple atrial automatic foci.

IST occurs in young, otherwise healthy patients who do not have reversible metabolic abnormalities, drug toxicities, or any other transient conditions producing the arrhythmia. Instead, IST is a chronic or persistent condition which is probably related to an underlying autonomic imbalance, and which can become quite debilitating over time. For all forms of automatic supraventricular tachycardias, the basic principle of therapy is to attempt to reverse the underlying cause. Digitalis toxicity should be suspected in any patient who has been taking this drug, and digitalis should be withheld until toxic levels are ruled out. If the ventricular response is rapid enough to produce hemodynamic instability, the ventricular rate can usually be slowed with digitalis (if toxicity has been ruled out), verapamil, or β blockers. In addition, if rapid 1 : 1 conduction is occurring during an automatic atrial tachycardia, an immediate slowing of the ventricular response can sometimes be accomplished by pacing the atria even faster than the rate of the tachycardia — fast enough to produce 2 : 1 or 3 : 1 AV block. Because these arrhythmias are not reentrant, they cannot be pace-terminated and usually do not respond well to direct current (DC) cardioversion. Class Ia antiarrhythmic drugs can be used in an attempt to terminate the arrhythmias; but, unless the underlying cause is reversed, these drugs tend to be relatively ineffective. The electrophysiology study offers no beneﬁt in patients with automatic supraventricular tachyarrhythmias.

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Reentrant supraventricular tachyarrhythmias

The vast majority of supraventricular tachyarrhythmias seen in ambulatory patients are due to reentry. In contrast to patients with automatic atrial tachycardias, reentrant supraventricular tachycardias are seen in patients who are not acutely ill. Further, in contrast to patients with reentrant ventricular tachyarrhythmias (see Chapter 7), reentrant supraventricular tachycardias are usually seen in patients who are free of chronic heart disease. Although reentrant circuits in the ventricle generally do not appear unless disease of the ventricular myocardium is present, the reentrant substrate for supraventricular arrhythmias tends to be congenital. Overt heart disease is therefore not necessary in order for a patient to develop these arrhythmias. Thus, the typical patient with reentrant supraventricular tachycardia is young and healthy. There are ﬁve general categories of reentrant supraventricular tachyarrhythmias: AV nodal reentry, bypass tract-mediated macroreentry, intraatrial reentry, SA nodal reentry, and atrial ﬂutter/atrial ﬁbrillation. Many clinicians still tend to lump these reentrant arrhythmias (except for atrial ﬂutter and atrial ﬁbrillation) together into one large group called PAT (paroxysmal atrial tachycardia — generally, any regular, narrow-complex tachycardia with sudden onset and sudden termination). The term PAT, however, is a vestige from the days when the mechanisms for supraventricular arrhythmias were poorly understood. Over the past 25 years, the electrophysiology study has made it clear that PAT is almost always due to one of the categories of reentrant supraventricular tachyarrhythmias just listed. In many cases, the knowledgeable clinician can tell which type of supraventricular tachyarrhythmia he or she is dealing with (and therefore what type of therapy to use) merely by keeping these categories in mind while examining a 12lead ECG of the arrhythmia. AV nodal reentrant tachycardia

AV nodal reentrant tachycardia is the most common type of reentrant supraventricular tachycardia and is the operative mechanism in up to 60% of patients presenting with PAT. In AV nodal reentry, the reentrant circuit is usually said to be enclosed within the AV node (Figure 6.2A). In patients with AV nodal reentry, the AV node is functionally divided into two longitudinal pathways (dual AV nodal pathways). These dual pathways form the reentrant circuit. Because, for all practical purposes, the reentrant circuit in AV nodal reentry involves the AV node exclusively, this arrhythmia responds well to autonomic maneuvers and drugs that affect the AV node (digitalis, calcium blockers, and β blockers).

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Fig. 6.2 The three most common reentrant supraventricular tachycardias. (A) AV nodal reentrant tachycardia. In this arrhythmia, the reentrant circuit is small and is thought to be localized entirely within the AV node. (B) Bypass tract-mediated macroreentrant tachycardia. An AV bypass tract serves as one pathway (usually the retrograde) and the normal AV conduction system serves as the other pathway of this large (hence, macroreentrant) reentrant circuit. (C) Atrial reentrant tachycardia. In this arrhythmia, the reentrant circuit is contained within the atrial myocardium.

Bypass tract-mediated macroreentrant tachycardia

Bypass tract-mediated macroreentrant tachycardia is the next most common type of arrhythmia presenting as PAT (30%). In macroreentrant tachycardia, an AV bypass tract is present. (The majority of patients presenting with macroreentrant tachycardia do not have overt WolffParkinson-White syndrome. Instead, they have concealed bypass tracts — bypass tracts that are incapable of conducting in the antegrade direction and therefore generate no delta waves.) In these patients, the bypass tract acts as one pathway (almost always the retrograde pathway), and the normal AV conducting system acts as the second pathway (the antegrade pathway) of the reentrant circuit (Figure 6.2B). Because this reentrant circuit is a large circuit involving the AV node, the His-Purkinje system, and the ventricular and atrial myocardia as well as the bypass tract, it is termed a macroreentrant circuit. Also, because the circuit consists of several types of cardiac tissue, it can be attacked on many levels by many types of drugs. Intraatrial reentry

Intraatrial reentry accounts for only a small percentage of patients presenting with PAT. In intraatrial reentry, the reentrant circuit is entirely within the atrial myocardium and does not involve the AV conducting system (Figure 6.2C). It resembles automatic atrial tachycardia in that discrete P waves, which usually differ from normal sinus P waves, precede each QRS complex, and AV block can occur without affecting

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the arrhythmia itself. It differs from automatic arrhythmias by its paroxysmal onset and offset and the fact that it can be induced and terminated by pacing. Class Ia drugs are often effective. Because the AV node is not part of the reentrant circuit, attacking the AV node does not affect this arrhythmia. SA nodal reentry

SA nodal reentry is a fairly uncommon arrhythmia in which the reentrant circuit is thought to be enclosed within the SA node. Discrete P waves identical to sinus P waves precede each QRS complex. SA nodal reentrant tachycardia is distinguishable from both normal sinus tachycardia and IST by its onset and termination, which is paroxysmal and does not display warm-up, and by its inducibility and terminability with pacing. Because the reentrant circuit is enclosed within the SA node, autonomic maneuvers and drugs such as digitalis, calcium blockers, and β blockers tend to ameliorate this arrhythmia. Atrial ﬂutter and atrial ﬁbrillation

Finally, atrial ﬂutter and atrial ﬁbrillation are forms of reentrant atrial tachycardias. These arrhythmias are generally distinctive enough not to be considered to be PAT by clinicians who still use this terminology. In atrial ﬂutter, the atrial rate is regular and in excess of 220 beats/min and usually displays a typical sawtooth pattern (Figure 6.3). Atrial ﬂutter can usually be terminated by pacing. Atrial ﬂutter is virtually always accompanied by AV block, usually in a 2 : 1 pattern. In atrial ﬁbrillation, the atrial activity is continuous and chaotic, and deﬁnite P waves cannot be distinguished (Figure 6.4). The ventricular response is irregular,

Fig. 6.3 Atrial ﬂutter. One surface ECG lead and the right atrial electrogram are shown. Note the rapid, regular atrial rate (cycle length approximately 200 msec) and the 2 : 1 ventricular response.

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Fig. 6.4 Atrial ﬁbrillation. Note the chaotic atrial activity, absence of discrete P waves, and irregularly irregular ventricular response.

reﬂecting the chaotic atrial activity. Both atrial ﬂutter and atrial ﬁbrillation are similar to intraatrial reentry (and to automatic atrial tachycardia), in that attacking the AV node does not directly affect these arrhythmias. In general, therapy is aimed at either converting the patient to normal sinus rhythm (with class I or class III drugs or cardioversion or both) or simply controlling the ventricular response with AV nodal blocking agents. In summary, reentrant supraventricular tachyarrhythmias include several types of arrhythmias, which have different therapies, depending on the location and characteristics of the respective reentrant circuits. Most of these arrhythmias are commonly lumped together as PAT, a practice that is counterproductive to appropriate therapy. Once these arrhythmias are understood, the proper diagnosis can often be made (and proper therapy initiated) without resorting to invasive testing. The electrophysiology study, however, can be vital in managing patients with reentrant supraventricular tachyarrhythmias, especially because the majority of these arrhythmias can now be cured with transcatheter ablation techniques (see Chapter 8).

General outline of the electrophysiology study in reentrant supraventricular tachyarrhythmias The key to studying supraventricular tachyarrhythmias in the electrophysiology laboratory is the capability of inducing these arrhythmias with programmed pacing techniques, while at the same time recording intracardiac electrograms from various key locations within the heart. As noted in Chapter 2, inducing any reentrant rhythm requires the existence of an appropriate anatomic substrate to form a reentrant circuit. In supraventricular tachyarrhythmias, the reentrant circuits can incorporate SA or AV nodal tissue, bypass tracts, and atrial and ventricular myocardial tissue. By recording strategically placed intra-

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cardiac electrograms and studying the patterns of activation, by examining the mode of initiation and termination of arrhythmias, and by studying the response to programmed pacing, most supraventricular tachyarrhythmias can be fully characterized in the electrophysiology laboratory. Speciﬁcally, the electrophysiology study seeks to determine the anatomic location and electrophysiologic characteristics of the reentrant circuit, the propensity of the circuit to sustain arrhythmias, the characteristics of those arrhythmias, and the response of the reentrant arrhythmias to various therapies. Positioning the catheters

To localize the reentrant circuits in supraventricular tachyarrhythmias, it is important to record electrograms from all four major cardiac chambers, as well as from the His bundle region. These recordings can generally be obtained by positioning four electrode catheters: One in the right atrium, one in the right ventricle, one in the His position, and one in the coronary sinus (to record both left atrial and left ventricular deﬂections; Figure 6.5). With catheters in these four positions, one can record electrograms from the most critical locations and introduce paced impulses from the right ventricle and from both atria (pacing from the coronary sinus catheter generally produces capture in the left atrium alone). Evaluation of supraventricular tachyarrhythmias

Once the catheters are positioned, the characteristics of the arrhythmia can be deduced by answering four general questions. First, what is the mode of initiation and termination of the tachycardia? Second, what are the patterns of antegrade and retrograde activation in sinus rhythm and during tachycardia? Third, what is the evidence that atrial or ventricular myocardium is necessary to the reentrant circuit? Fourth, what are the effects of autonomic maneuvers and drugs on the tachycardia? These questions must be addressed for each type of supraventricular tachycardia that is induced during the study. What is the mode of initiation and termination of the tachycardia?

In assessing the mode of initiation of tachycardia, the electrophysiologist addresses several points. First, is the tachycardia more readily inducible from one location than another? As noted in Chapter 4, inducing a reentrant arrhythmia requires the delivery of a premature impulse to the reentrant circuit at just the right moment. A major element inﬂuencing the inducibility of reentrant arrhythmias, then, is the distance between the pacing catheter

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Fig. 6.5 Baseline recordings during a typical electrophysiology study for supraventricular tachycardia. Surface leads I, II, and V1 allow estimation of the QRS axis. The high right atrial electrogram (HRA) records activity near the SA node. The His bundle electrogram is recorded from several electrode pairs on the His catheter (three in this example). Two recordings are made from the coronary sinus (both of which record left atrial and left ventricular activity) — coronary sinus distal (CSD) is recorded from the distal electrode pair on the coronary sinus catheter, and coronary sinus proximal (CSP) is recorded from the proximal pair of electrodes. Finally, a recording is made from the right ventricular apex (RVA). With this combination of recordings, the electrophysiologist can keep track of events in all four cardiac chambers, as well as in the normal AV conducting system.

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and the reentrant circuit — the closer the catheter is to the circuit, the more likely it is that a paced premature beat will arrive at the circuit early enough to induce reentry. Thus, for instance, if a reentrant rhythm is signiﬁcantly easier to induce with left atrial pacing (i.e., pacing from the coronary sinus) than it is with right atrial pacing, then the reentrant circuit may be expected to involve a left-sided bypass tract. It is important to observe whether supraventricular tachycardia is readily inducible with ventricular pacing. Inducing tachycardia with ventricular pacing is readily accomplished in macroreentrant tachycardias, is relatively difﬁcult in AV nodal reentry, and is rare with intraatrial reentry. (In intraatrial reentry, the arrhythmia can be induced by ventricular stimulation only indirectly and infrequently, by means of retrograde stimulation of the atrium.) Another point relating to the mode of initiation of the tachycardia is the site of the conduction delay that typically occurs with the onset of reentrant supraventricular tachyarrhythmias. The reason for this conduction delay can be seen by reviewing the mechanism of inducing reentrant arrhythmias (see Figure 2.6). As described in Chapter 2, a reentrant circuit requires two roughly parallel pathways (labeled pathways A and B) connecting proximally and distally to common conducting tissues, forming an anatomic circuit. Pathway B has a longer refractory period than pathway A, and pathway A conducts impulses slower than pathway B. The initiation of reentry occurs when a premature impulse enters the circuit at a time when pathway B is still refractory from the previous normal impulse but pathway A has already recovered. Note that, since pathway B conducts faster than pathway A, a normal (i.e., not premature) impulse will conduct via pathway B rather than pathway A (Figure 6.6A). When an early impulse initiates reentry, this impulse is blocked in pathway B (the fast pathway) and instead conducts via pathway A (the slow pathway). Thus, a beat that initiates reentry, is commonly accompanied by conduction delay (Figure 6.6B). The electrophysiologist must pay particular attention to the occurrence of conduction delay in association with the onset of tachycardia. The site of this delay virtually always points to one of the pathways within the reentrant circuit. An additional issue relating to the mode of initiation is the tachycardia (or echo) zone. The tachycardia zone is the range of coupling intervals of premature beats that will initiate reentrant tachycardia. As one introduces a series of premature impulses with progressively shorter coupling intervals, one impulse will eventually encounter the reentrant circuit during the effective refractory period (ERP) of pathway B (i.e., the impulse blocks in pathway B). At this point, reentry is often initi-

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Fig. 6.6 Why reentry is accompanied by a conduction delay. (A) In this generic reentrant circuit, a normal impulse travels from top to bottom by the fastest available pathway (pathway B). No conduction delay is seen. (B) When a premature impulse blocks in pathway B and initiates reentry, that impulse now travels from top to bottom via the slow pathway (pathway A). Thus, an observer watching the exit of the impulse from the circuit will see a conduction delay whenever reentry is initiated.

ated. The latest premature impulse that blocks in pathway B (if it were any later the impulse would not encounter refractory tissue) usually deﬁnes the beginning of the tachycardia zone. If one now continues to introduce premature impulses with progressively shorter coupling intervals, reentry will typically be induced with each succeeding premature beat until the ERP of pathway A is ﬁnally encountered. At this point, the premature impulse blocks in both pathways of the reentrant circuit and no further reentry occurs. The ERP of pathway A thus deﬁnes the end of the tachycardia zone. Note that the width of the tachycardia zone is related to the difference between the refractory periods of the two pathways constituting the reentrant circuit. The wider the tachycardia zone, the more likely a premature impulse will fall within that zone and

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induce reentry. During the electrophysiology study for supraventricular tachycardia, one thus tries to identify the refractory periods (and thus the tachycardia zone) of the various pathways involved in the reentrant circuit. By doing so, one can attempt to tailor therapy to reduce the width of the tachycardia zone. The mode of termination of the arrhythmia is somewhat less helpful than the mode of initiation in localizing the bypass tract. Nonetheless, careful observation of the precise mechanism of termination of reentry can offer clues as to the type of reentrant rhythm. This point will be discussed in detail later. What are the patterns of antegrade and retrograde activation during sinus rhythm and during supraventricular tachycardia?

Abnormalities in the pattern of activation of impulses traveling from the atria to the ventricles and from the ventricles to the atria can help to localize portions of the reentrant circuit. We have already discussed normal antegrade activation patterns (see Chapter 1). Impulses arising in the SA node traverse the atria in a radial fashion until they encounter the ﬁbrous skeleton of the heart at the AV groove. There, the impulses are abolished except in the AV conducting system (the AV node and His-Purkinje structures). Because of its electrophysiologic properties, impulses conduct relatively slowly through the AV node. Further, premature impulses conduct even more slowly (manifested in the His electrogram as a prolonged AH interval). Typically, if one introduces single atrial extrastimuli with progressively shorter coupling intervals, the delay in AV nodal conduction (and the AH interval) increases gradually. Eventually, the ERP of the AV node is reached and the early impulse is blocked. This normal pattern of gradually increasing AH intervals with progressively premature atrial impulses is shown graphically in Figure 6.7. This AV nodal conduction curve shows the normal smooth and continuous prolongation in AH intervals with progressively premature beats. This normal pattern can be disrupted by two general conditions that produce supraventricular tachycardias: Dual AV nodal pathways and AV bypass tracts. These two conditions will be discussed in detail later. When an impulse is conducted from the atria to the ventricles via the normal AV conducting system, ventricular activation follows a typical pattern. First, the intraventricular septum is depolarized, then the apices of the right and left ventricles, then the ventricular free walls, and ﬁnally the basilar portions of the ventricles. The area of the ventricles that is depolarized last is the left ventricular posterobasilar area. This normal pattern of ventricular activation is altered if there is a bypass

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Fig. 6.7 A normal AV conduction curve. With progressively shorter coupling intervals, premature atrial beats display a progressive conduction delay in the AV node. In this graph, the conduction intervals (A1A 2) are shown on the x axis, and the resulting AH intervals (A2H2) are shown on the y axis. The normal AV conduction curve is smooth and continuous, as shown.

tract that preexcites the ventricle. Studying the ventricular activation pattern in the electrophysiology laboratory can help to localize the ventricular insertion of a bypass tract. The characteristics of normal retrograde conduction (i.e., the conduction of impulses from the ventricles to the atria that occurs during ventricular pacing) are important in evaluating supraventricular tachycardias. Normally, retrograde conduction occurs over the normal AV conducting system — the impulse travels from the ventricular myocardium to the Purkinje ﬁbers, then to the His bundle, to the AV node, and ﬁnally to the atria, where it spreads in a radial fashion (i.e., from the atrial septum to the right and left atria). Although some retrograde conduction can be seen in most individuals, in most cases retrograde conduction is not as efﬁcient as antegrade conduction. Thus, in most individuals, retrograde block occurs at longer coupling intervals than antegrade block. (This is not always the case, however — e.g., a substantial minority of patients with complete AV block have intact retrograde conduction.) In normal individuals, if one introduces progressively earlier extrastimuli from the ventricle and measures the retrograde conduction

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intervals, one will see a progressive prolongation of the VA interval (Figures 6.8 and 6.9), similar to the gradual prolongation in the AH interval that one sees with antegrade conduction. Normally, block will occur ﬁrst in the His-Purkinje system. In practical terms, however, one is only rarely able to discern the H spike in the His electrogram during retrograde conduction, as it is usually hidden in the large V complex. In studies of supraventricular tachyarrhythmias, the pattern of retrograde atrial activation is important. With normal retrograde conduction, the earliest atrial activation is seen in the His electrogram because that electrogram records the atrial activity near the AV node (i.e., the point of entry of the impulse into the atrial myocardium during normal retrograde conduction). The retrograde impulse then spreads radially across the atria, and the right atrial electrogram and left atrial electrogram are inscribed more or less at the same time (Figure 6.10A). This normal pattern of retrograde activation can be disrupted if an AV bypass tract is present. In this case, eccentric retrograde activation of the atria can occur. With a right-sided bypass tract, for instance, the right atrial electrogram will be inscribed earliest (Figure 6.10B); with a left-sided bypass tract, the left atrial electrogram will be inscribed earliest (Figure 6.10C). Mapping of retrograde atrial activation is one of the most useful methods of localizing AV bypass tracts.

Fig. 6.8 Normal VA conduction during right ventricular pacing, A. Figs. 6.8 and 6.9 show the characteristics of normal retrograde conduction during ventricular pacing using the extrastimulus technique. Each ﬁgure shows a surface ECG lead, a high right atrial (HRA) electrogram, and a His bundle electrogram. With a relatively long S1–S2 coupling interval, retrograde conduction to the atrium is rapid (the VA interval following the S2 is short). Note that the retrograde atrial impulse is recorded in the His electrogram (near the AV node) before it reaches the high right atrium. This suggests retrograde conduction via the normal AV conducting tissues.

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Fig. 6.9 Normal VA conduction during right ventricular pacing, B. With a shorter coupling interval, retrograde conduction still occurs, but is slower (the VA interval following the S2 is longer than in the previous ﬁgure). This retrograde conduction delay with shorter coupling intervals is normal when retrograde conduction occurs via the normal AV conducting tissues.

Fig. 6.10 Patterns of retrograde atrial activation. Patterns of retrograde atrial activation are important for localizing AV bypass tracts. This ﬁgure shows electrograms from the high right atrium (HRA), the His bundle, the coronary sinus (CS), and the right ventricular apex (RVA) during pacing from the RVA. (A) The normal pattern of retrograde atrial activation. This pattern is seen when retrograde conduction occurs via the normal AV conducting system or with septal bypass tracts. The atrial septum is activated ﬁrst (His electrogram), followed by left atrial (CS electrogram) and right atrial activation. (B) Retrograde activation pattern with a right-sided bypass tract. The right atrium is activated ﬁrst because retrograde conduction occurs via a right-sided bypass tract. The septal atrium and the left atrium are then activated. (C) Retrograde activation pattern with a left-sided bypass tract. The left atrium is activated ﬁrst (CS electrogram) because retrograde conduction occurs via a left-sided bypass tract. The atrial septum and the right atrium are then activated.

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What is the evidence that atrial or ventricular myocardium is necessary to the reentrant circuit?

Once a reentrant tachycardia has been induced, it can be helpful to attempt to deduce whether the atrial myocardium and ventricular myocardium are part of the reentrant circuit. One should always look for evidence of antegrade or retrograde block during the tachycardia. If either antegrade or retrograde block is seen to occur without affecting the cycle length of the tachycardia, macroreentry can be essentially ruled out. For instance, in AV nodal reentrant tachycardia, retrograde stimulation of the atria occasionally occurs with a Wenckebach pattern (i.e., occasional retrograde beats are dropped). When this phenomenon is observed during a supraventricular tachycardia of constant cycle length, a reentrant circuit in which the atria are required for the maintenance of tachycardia can be ruled out. The effect of bundle branch block on the cycle length of the tachycardia can also be instructive. In AV nodal reentry, bundle branch block does not change the reentrant circuit because the circuit does not involve the bundle branches. In macroreentry, however, the sudden occurrence of bundle branch block on the same side as the AV bypass tract (such as left bundle branch block occurring during a macroreentrant tachycardia involving a left-sided bypass tract) will increase the cycle length of the tachycardia (Figure 6.11). What are the effects of autonomic maneuvers and drugs on the tachycardia?

When attempting to deﬁne the anatomic substrate of, and effective therapy for, reentrant supraventricular tachyarrhythmias, it is often helpful to take advantage of the differential effects of autonomic maneuvers and drugs on various cardiac structures. As noted in previous chapters, the AV node has rich autonomic innervation and is exquisitely sensitive to changes in both sympathetic and parasympathetic tone. In contrast, atrial and ventricular myocardial tissue responds moderately to changes in sympathetic tone but only minimally to changes in parasympathetic tone. Thus, vagal maneuvers, by increasing the refractory period and decreasing the conduction velocity of the AV node, can terminate reentrant arrhythmias in which the AV node is part of the reentrant circuit (such as AV nodal reentry and macroreentry). If the AV node is excluded from the reentrant circuit (as in intraatrial reentry), vagal maneuvers may increase heart block but will not directly alter the reentrant impulse. Likewise, drugs that have a speciﬁc effect on the AV node (such as digitalis, calcium blockers, and β blockers) can be effective in terminating

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Fig. 6.11 Effect of bundle branch block on macroreentrant tachycardia. In this ﬁgure, macroreentrant tachycardia involving a left-sided bypass tract is present. Initially, no bundle branch block is present, and the tachycardia cycle length is 380 msec. If left bundle branch block occurs, it will now take longer for the reentrant impulse to reach the left-sided bypass tract, and the tachycardia cycle length is prolonged to 440 msec.

or preventing reentrant arrhythmias that include the AV node as part of the circuit. In contrast, class Ia drugs have relatively little effect on the AV node but increase the refractory periods and slow conduction velocity in atrial and ventricular myocardium and in bypass tracts. Thus, reentrant circuits that involve these structures can be altered by class Ia drugs. Class Ib drugs affect the ventricular myocardium (and bypass tracts) but not atrial myocardium or the AV node. Because some supraventricular tachycardias (i.e., macroreentry) involve ventricular myocardium, the class Ib drugs may be useful in some cases. The class Ic drugs slow conduction in all cardiac tissues, including AV node. Although offering relatively little help in identifying the anatomic substrate, class Ic drugs can be helpful in treating many forms of supraventricular tachyarrhythmias. General procedure for performing the electrophysiology study in patients with supraventricular tachyarrhythmias

When studying patients with supraventricular tachyarrhythmias, after the electrode catheters are in position most electrophysiologists begin with ventricular stimulation to study the characteristics of retrograde

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conduction. Although it may seem odd to begin with ventricular pacing when studying supraventricular arrhythmias, there are two reasons for doing so. First, many patients who have supraventricular tachycardias (especially those with bypass tracts) have the propensity for developing atrial ﬁbrillation with atrial pacing. Atrial ﬁbrillation, by its nature of continuous and chaotic atrial activity, virtually precludes meaningful evaluation of other reentrant supraventricular arrhythmias. By ﬁrst performing ventricular stimulation, the electrophysiologist hopes to avoid the early induction of atrial ﬁbrillation. Second, for AV nodal reentry and for bypass tract-mediated macroreentry (the two most common forms of reentrant supraventricular tachyarrhythmias), retrograde conduction is a prominent and necessary component of reentry. Thus, the characteristics of retrograde conduction and the retrograde activation pattern of the atrium with ventricular stimulation are important in characterizing these arrhythmias. It is therefore logical to evaluate these characteristics as early as possible. Generally, retrograde conduction is evaluated using the extrastimulus and incremental pacing techniques. Single ventricular extrastimuli are introduced (either in sinus rhythm or following a train of paced beats) with gradually decreasing coupling intervals until the extrastimulus fails to capture the ventricle. With each extrastimulus, the electrophysiologist notes the presence or absence of retrograde stimulation of the atrium, the pattern of atrial activation, and the conduction time of the retrograde impulse (the VA interval; see Figures 6.8 and 6.9). The coupling interval at which retrograde conduction is blocked (the retrograde ERP) is also noted. Next, incremental trains are introduced with progressively shorter cycle lengths. Note is taken of the cycle length at which 1 : 1 retrograde conduction no longer occurs. After ventricular stimulation is completed, pacing is performed from the high right atrium. The procedure here is similar to that described in Chapter 5 — atrial extrastimuli and incremental atrial pacing are used to assess the characteristics of AV conduction and of SA nodal function. Next, similar stimulation is performed using left atrial pacing (i.e., with the coronary sinus catheter). This is done to look for evidence of a left-sided AV bypass tract. When a bypass tract is suspected, pacing from multiple atrial sites is often performed (by moving the right atrial and/or coronary sinus catheters to various positions) to try to localize the bypass tract — the closer to the bypass tract one paces, the more preexcitation will occur. For the vast majority of patients with reentrant supraventricular tachyarrhythmias, the reentrant arrhythmia will be induced during one or more of these pacing maneuvers. Whenever reentrant tachycardia is

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induced, the protocol is interrupted so that the characteristics of the arrhythmia can be studied. Speciﬁcally, the mechanism of the tachycardia is noted, the cycle length is recorded, an assessment of the patient’s hemodynamic stability and level of symptoms is made, and atrial or ventricular stimulation is carried out to examine the effect of such stimulation on the arrhythmia. If reentrant supraventricular tachycardia is not induced with standard pacing techniques, multiple extrastimuli are used and drug administration (such as an isoproterenol infusion) is implemented to try to bring out the arrhythmia. If a bypass tract is known or suspected to occur, the ﬁnal step during the baseline (drug-free) study is to induce atrial ﬁbrillation. This is done to assess the ability of the bypass tract to conduct rapidly enough during atrial ﬁbrillation to pose a lethal risk to the patient. Finally, at the end of the baseline study, after the reentrant circuits have been localized and the mechanism of tachycardia has been deduced, drug studies may be carried out in an attempt to devise effective therapy for the patient. Drug studies for supraventricular tachycardias, however, are becoming ever more rare, now that most of these arrhythmias are routinely treated with ablation procedures. Although this general outline of the electrophysiology study for supraventricular tachyarrhythmias is fairly representative, no two electrophysiologists follow precisely the same protocol. In fact, no single electrophysiologist follows precisely the same protocol in every patient. Even within the same general category of arrhythmias, supraventricular arrhythmias show tremendous variability from patient to patient. Thus, every electrophysiology study has to be individualized. Electrophysiologists usually approach these patients with a general outline of a protocol, tailoring the study as they go, depending on the ﬁndings. With this introduction, we will now review the electrophysiologic evaluation of speciﬁc types of supraventricular tachyarrhythmias.

The electrophysiology study in AV nodal reentrant tachycardia As we have noted, AV nodal reentrant tachycardia is the most common type of arrhythmia presenting as PAT, probably accounting for 60% of all such arrhythmias. AV nodal reentry is seen in all age groups and occurs in both sexes equally. The incidence of underlying heart disease in patients with this arrhythmia is no greater than in the normal population.

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Mechanism of AV nodal reentry

One can think of the AV node in patients with AV nodal reentrant tachycardia as being shaped like a doughnut (Figure 6.12). The AV node in these patients behaves functionally as if there were two separate pathways through the node. The two pathways (the alpha and the beta pathways) are differentiated by their characteristic electrophysiologic properties. The alpha pathway (or the slow pathway) usually has a relatively short ERP and conducts slowly. The beta pathway (or the fast pathway) usually has a relatively long ERP and conducts more rapidly. Patients whose AV nodes are arranged in such a fashion are said to have dual AV nodal pathways. (See Chapter 8 for a more detailed discussion of the anatomy and physiology of dual AV nodal pathways.) In patients with dual AV nodal pathways, a normally timed sinus impulse will conduct through the AV node via the beta pathway, since the beta conducts more rapidly than the alpha pathway (Figure 6.12A).

Fig. 6.12 AV nodal reentrant tachycardia. (A) In AV nodal reentry, the AV node is functionally divided into two pathways (alpha α and beta β). The alpha pathway conducts more slowly than the beta, and the beta pathway has a longer refractory period than the alpha. A normal atrial impulse reaches the ventricles via the beta pathway. (B) A premature atrial impulse can ﬁnd the beta pathway refractory at a time when the alpha pathway is not refractory. In this case, the premature impulse conducts via the alpha pathway. Because conduction down the alpha pathway is slow, the resultant PR interval is prolonged. (C) If conditions are right, a premature impulse can block in the beta pathway and travel down the alpha pathway (as in B), then travel retrograde up the beta pathway and reenter the alpha pathway in the antegrade direction. A circuitous impulse is thus established within the AV node, and AV nodal reentrant tachycardia results. Note the prolonged PR interval in the beat that starts AV nodal reentry (caused by jumping from the beta to the alpha pathway). This conduction delay is typically seen in reentrant supraventricular arrhythmias.

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However, a premature atrial impulse can arrive at the AV node at such a time that the beta pathway (with a relatively long ERP) is still refractory from the previous normal beat, but the alpha pathway (with a relatively short ERP) is no longer refractory. This early impulse will then traverse the alpha pathway, reaching the His bundle after a prolonged conduction time through the AV node (since the alpha pathway conducts slowly [Figure 6.12B]). This AV nodal conduction delay is manifested by a prolonged PR interval on the surface ECG. If the beta pathway recovers by the time the impulse reaches the distal portion of the alpha pathway, the impulse may conduct retrogradely up the beta pathway (producing an atrial echo beat). If this retrograde impulse is then able to reenter the alpha pathway, a continuously circulating impulse can be established within the AV node. This is AV nodal reentrant tachycardia (Figure 6.12C). Thus, in AV nodal reentrant tachycardia, the reentrant circuit is located within the AV node. In most cases, both the atria and the ventricles are stimulated by impulses exiting from the circuit during each lap. Neither the atria nor the ventricles, however, are necessary for the maintenance of that reentrant circuit. It is thus possible to have block in the His bundle, preventing the ventricles from being stimulated, without affecting the reentrant circuit itself. It is also possible to have retrograde block, preventing the atria from being stimulated, but without affecting the arrhythmia. There is evidence that in some patients the beta pathway may not be typical AV nodal tissue. In such patients, the beta pathway does not respond to AV nodal drugs (digitalis, calcium blockers, β blockers) as well as the alpha pathway. In these patients, the beta pathway may be more affected by class Ia drugs than is typical for AV nodal tissue. Mode of initiation and termination of AV nodal reentry

Most often, AV nodal reentrant tachycardia is induced with atrial extrastimuli. If one introduces progressively earlier atrial premature impulses, impulses with relatively longer coupling intervals will conduct down the beta (fast) pathway, just as sinus beats do (Figure 6.13). When the coupling interval of a premature impulse, however, becomes shorter than the ERP of the beta pathway, that impulse blocks in the beta pathway and jumps to the alpha (slow) pathway (thus producing the typical conduction delay in the AV node). It is at this point that AV nodal reentry is usually ﬁrst seen (Figure 6.14). Premature impulses that are yet earlier will also induce AV nodal reentry, until the ERP of the alpha pathway is reached (at which point the premature impulse is blocked entirely). The tachycardia zone in AV nodal reentry is from the ERP of the beta pathway

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Fig. 6.13 Initiation of AV nodal reentry with atrial extrastimuli, A. Figures 6.13 and 6.14 demonstrate the induction of AV nodal reentry using the atrial extrastimulus technique. In both ﬁgures, one surface ECG lead, one high right atrial electrogram, and one His bundle electrogram are shown. In this ﬁgure, an S2 impulse conducts through the normal AV conducting system with a moderate prolongation in the AH interval. This response is normal and is similar to the normal conduction pattern shown in Figs. 5.20 and 5.21.

Fig. 6.14 Initiation of AV nodal reentry with atrial extrastimuli, B. With a slightly shorter S1–S2 coupling interval, a large jump in the resultant AH interval occurs (compared to the previous ﬁgure), and AV nodal reentry is initiated. The sudden increment in AH intervals represents a shift in conduction from the beta to the alpha pathway in this patient with dual AV nodal pathways. Note (in the last two beats in this ﬁgure) that during AV nodal reentry, the retrograde A spike (which is labeled on the His electrogram) occurs very soon after the V spike. This is because retrograde conduction occurs via the rapidly conducting beta pathway. On the surface ECG the retrograde P wave is usually buried in the QRS complex (as in this ﬁgure) during AV nodal reentrant tachycardia.

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to the ERP of the alpha pathway. In this arrhythmia, the tachycardia zone tends to be quite reproducible (that is, successive measurements will yield the same result). Atrioventricular nodal reentry is also commonly induced with incremental atrial pacing at the Wenckebach cycle length. At this cycle length, progressive prolongation in AV nodal conduction is seen until block occurs in the beta pathway and conduction occurs instead down the alpha pathway — at this point, AV nodal reentry is usually seen. Atrioventricular nodal reentry is less often, and less reproducibly, induced with ventricular pacing. Normally in patients with dual AV nodal pathways, ventricular pacing produces retrograde impulses that enter the AV node and begin traveling up both the beta and alpha pathways (Figure 6.15A). Because conduction in the beta pathway is faster, the retrograde impulse reaches the atria via the beta pathway. Reentry is not induced, however — the impulse is not able to turn around and travel back down the alpha pathway because the alpha pathway has just been stimulated itself by the retrograde impulse and is still refractory. Relatively rarely, AV nodal reentry is induced by ventricular pacing if a ventricular extrastimulus can be interpolated between two sinus beats. In this case, the beta pathway can be rendered refractory by the retrograde impulse, so that the next sinus impulse blocks in the beta pathway and conducts down the alpha pathway, thus producing reentry (Figure 6.15B). Termination of AV nodal reentrant tachycardia follows the typical pattern described in Chapter 4 (see Figure 4.11). Relatively late premature impulses can encounter refractory tissue and be prevented from entering the circuit (see Figure 4.11A). Early impulses may enter the circuit via the alpha pathway, resulting in a resetting of the tachycardia (see Figure 4.11B). Yet earlier impulses can terminate the tachycardia (see Figure 4.11C). The ability to cause a premature impulse to reach the AV node early enough to terminate AV nodal reentry depends on the distance of the pacing catheter from the AV node and on the refractory and conduction characteristics (i.e., the functional refractory period [FRP] — see Chapter 4) of the intervening tissue. If terminating the tachycardia with single atrial or ventricular extrastimuli is not possible, one can improve the chances of terminating the arrhythmia by repositioning the catheter or, more commonly, by introducing multiple extrastimuli. This latter maneuver has the effect of reducing the FRP of intervening myocardial tissue. Patterns of activation with AV nodal reentry

Dual AV nodal pathways are the rule in patients with AV nodal reentrant tachycardia. Because there are two pathways of conduction through the

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Fig. 6.15 Initiation of AV nodal reentry with a ventricular paced beat. Because the reentrant circuit in AV nodal reentry is exposed to both the atria and the ventricles, it is possible that a premature ventricular beat (as well as a premature atrial beat) can initiate reentry. However, in practice this event is rare. (A) A ventricular paced impulse begins traveling up both the beta β and alpha α pathways. The impulse reaches the atria via the beta pathway (since this pathway conducts rapidly) and cannot reenter the alpha pathway because it encounters the retrograde impulse traveling slowly up the alpha pathway. This is why AV nodal reentry is difﬁcult to initiate with ventricular pacing. (B) If the events shown in (A) occur at just the right time, the following sinus beat can encounter the AV node at a time when the beta pathway is still refractory from the recent retrograde impulse. Thus, AV nodal reentry can be initiated indirectly by a premature ventricular impulse.

AV node, the AV nodal conduction curve can be expected to be abnormal. Figure 6.16 shows a typical AV nodal conduction curve in a patient with dual AV nodal pathways. With extrastimuli having relatively long coupling intervals, conduction through the AV node occurs via the beta pathway. As atrialextrastimuli are introduced with progressively shorter coupling intervals, the AH interval increases gradually at ﬁrst, as it would in a normal AV node. At the point at which the ERP of the beta pathway is reached, however, conduction suddenly shifts to the alpha pathway, at which time there is a sudden increment in the AV nodal conduction time. This increment is manifested by a sudden jump in the AH interval. The AV nodal conduction curves in patients with dual AV nodal

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Fig. 6.16 A typical AV conduction curve from a patient with AV nodal reentrant tachycardia. Compare this curve to the normal curve in Fig. 6.7. In AV nodal reentry, dual AV nodal pathways are present. Premature atrial impulses with longer coupling intervals conduct down the beta pathway. With earlier premature atrial impulses, the refractory period of the beta pathway is reached, and conduction jumps to the slower alpha pathway. It is at this point that AV nodal reentry may occur. On the AV conduction curve, this jump from faster to slower conduction is manifested by a sudden discontinuity in the curve. The sudden lengthening of the AH interval when conduction shifts from the beta to the alpha pathway is also seen in Figs. 6.13 and 6.14.

pathways show a discontinuity — the discontinuity represents the point at which conduction shifts from the beta to the alpha pathway. Occasionally, patients with dual AV nodal pathways will manifest their two pathways during normal sinus rhythm — these patients can be seen to have two distinct PR intervals during sinus rhythm. In other patients with dual AV nodal pathways, evidence for dual pathways is not seen during baseline electrophysiologic testing. In these patients, the ERPs of the alpha and beta pathways are similar (i.e., the tachycardia zone is extremely narrow). Such patients either have few arrhythmias or only have arrhythmias when autonomic stresses (such as a sympathetic surge) dissociate the refractory periods of the two pathways (in which case a differential effect of autonomic stresses on the two pathways must be postulated). When AV nodal reentry is suspected in patients who have no evidence for dual pathways during baseline testing, autonomic

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or pharmacologic maneuvers should be tried in an attempt to dissociate the pathways. The pattern of ventricular activation during antegrade conduction is normal because stimulation of the ventricles in AV nodal reentry is via the normal His-Purkinje system. Likewise, the pattern of atrial activation during retrograde stimulation is also normal. Evidence that atrial and ventricular myocardium are not required for AV nodal reentry

Most authorities feel that atrial and ventricular myocardium are not necessary for maintenance of AV nodal reentry. Although during electrophysiologic testing it is difﬁcult to prove that atrial and ventricular tissues are not required to maintain AV nodal reentry, evidence is sometimes present spontaneously during AV nodal reentrant tachycardia. One should always be alert for the phenomenon of retrograde Wenckebach conduction during tachycardia. If the tachycardia cycle length is constant at the same time that the relationship of the retrograde P waves to the QRS complex is changing, or especially if occasional retrograde P waves are dropped, that is strong evidence that the atria are not required for the maintenance of the tachycardia. Likewise, if occasional antegrade block occurs without a change in the tachycardia cycle length, the ventricles are thus not required for maintenance of tachycardia. Finally, because the activation pattern of the ventricular myocardium has no bearing on the cycle length of the reentrant circuit, if bundle branch block should develop during AV nodal reentry, no change in the rate of the tachycardia should occur. If these spontaneous events are not seen, then extrastimuli from the atria and the ventricles can help to show that the atria and ventricles are not required. Capture of the atria near the AV node or capture of the His bundle without changing the tachycardia suggests that the reentrant circuit is localized to the AV node. In practice, it is difﬁcult and impractical to prove that the atria and the ventricles are not necessary by using extrastimuli. Fortunately, it is also usually unnecessary because the diagnosis of AV nodal reentry rarely hinges on the rigorous documentation that the atria and ventricles are not required. Other observations in AV nodal reentry Relationship of P waves to QRS complexes during AV nodal reentry

One of the most useful observations made in the electrophysiology laboratory in patients with AV nodal reentry is the relationship between retrograde P waves and the QRS complexes on the surface ECG during the tachycardia. During AV nodal reentry, the atrium is stimulated in

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the retrograde direction by impulses exiting to the atria via the beta pathway. Because the beta pathway tends to conduct rapidly, retrograde atrial activation tends to occur during or just after ventricular depolarization. On the surface ECG, P waves thus tend either to be buried within the QRS complex or to occur just at the end of the QRS. In patients presenting with regular, narrow-complex tachycardia in which P waves cannot be discerned at all in a good-quality 12-lead ECG, one can make the diagnosis of AV nodal reentry with some conﬁdence. Atypical AV nodal reentry

In patients with atypical AV nodal reentry, the ERP of the alpha pathway is longer than that of the beta pathway. In these individuals, reentry occurs in the opposite direction (i.e., up the alpha pathway and down the beta pathway), and the P to QRS relationship is not typical of AV nodal reentry (because retrograde conduction occurs through the slow pathway). Patients with this unusual form of AV nodal reentry tend to have incessant tachycardia. Treatment of AV nodal reentry

Because both pathways in AV nodal reentry involve AV nodal tissue, drugs and maneuvers that increase the refractory period and slow the conduction velocity of AV nodal tissue are very effective at terminating the arrhythmia. In addition to maneuvers that increase vagal tone (the Valsalva maneuver, carotid sinus massage, and ice water immersion), the digitalis agents, calcium blockers, and β blockers tend to be effective. In most instances, these agents work by producing Wenckebach conduction in the slow pathway. They thus cause termination of reentrant tachycardia after a few cycles, when an impulse that has conducted retrogradely through the beta pathway fails to reenter the alpha pathway. Because occasionally the alpha and beta pathways respond differently to various agents, it is sometimes possible to potentiate tachycardia with drugs. For instance, in some patients, the beta pathway is relatively unaffected by drugs that normally depress AV nodal function. Thus, a drug might slow conduction in the alpha pathway without prolonging refractoriness in the fast pathway. In this case, any premature impulse traveling down the alpha pathway would tend to be so delayed that the beta pathway would be much more likely to have recovered by the time the impulse reaches it. Reentry, then, would tend to be easier to start and more difﬁcult to stop. Patients in whom standard AV nodal drugs seem to be ineffective may respond to class Ia or class Ic drugs. The beta pathway in such

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patients seems to behave less like AV nodal tissue and more like atrial or ventricular myocardial tissue. During the last 15 years, techniques for performing transcatheter ablation of the slow (alpha) pathway in patients with AV nodal tachycardia have become quite advanced (see Chapter 8). Transcatheter ablation of AV nodal reentry can now be performed successfully in well over 95% of patients who undergo this procedure. Ablation should be strongly considered in any patient with AV nodal reentry who has frequent or disabling episodes.

Bypass tract-mediated supraventricular tachyarrhythmias As described in Chapter 1, there is normally only one way for electrical impulses to travel from the atria to the ventricles — that is by the normal AV conduction system. Of every thousand individuals, however, several are born with a second electrical connection between the atria and the ventricles. These extra connections are called bypass tracts (or accessory pathways), because they offer a potential route for electrical impulses to bypass the normal AV conduction system. Bypass tracts consist of tiny bands of myocardial tissue that most commonly insert in atrial muscle on one end and in ventricular muscle on the other end. They tend to occur sporadically in the normal population, although patients with Ebstein’s anomaly and mitral valve prolapse have a somewhat higher incidence than the general population. The electrophysiologic characteristics of these bypass tracts vary, but they generally behave much more like myocardial tissue than AV nodal tissue. Thus, they do not display slowing of conduction with premature impulses as the AV node does. Also, when stimulated rapidly, bypass tracts develop block in the manner of His-Purkinje tissue rather than AV nodal tissue. That is, the block is sudden (of the Mobitz II variety) instead of gradual (i.e., Wenckebach conduction does not occur). Bypass tracts are generally invisible to the naked eye (signiﬁcantly, surgeons cannot see them when attempting surgical disruption) and therefore must be located by their electrophysiologic effects alone. Bypass tracts can occur virtually anywhere along the AV groove (except in the space between the aortic valve and the mitral valve) and can also occur more or less parallel to the AV conducting system in the septal area. There are four general types of bypass tracts (Figure 6.17): AV bypass tracts (the “typical” bypass tracts, in which the tract is located along the AV groove and connects atrial and ventricular muscle; Figure

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Fig. 6.17 Four types of bypass tracts. Tract A is an AV bypass tract, connecting atrial myocardium to ventricular myocardium. Tract B is an AV nodal bypass tract, connecting atrial myocardium to the His-Purkinje system. Tract C is a “Mahaim” tract, connecting the distal atrium (near the AV node) to the right bundle branch. Tract D connects the distal conducting system to the ventricular myocardium.

6.17, tract A); AV nodal bypass tracts (which connect the low atrial myocardium to the His-Purkinje system; tract B); bypass tracts that connect the distal atrial myocardium (near the AV node) to the right bundle branch (so-called “Mahaim” tracts; tract C); and bypass tracts that connect the His or Purkinje ﬁbers to ventricular myocardium (tract D). AV bypass tracts are by far the most common variety. Bypass tracts may or may not conduct in the antegrade direction. When they do (in which case the patient is said to have Wolff-ParkinsonWhite syndrome), the surface ECG often shows preexcitation of the QRS complex (Figures 6.18 and 6.19). Preexcitation refers to antegrade conduction over a bypass tract that stimulates the ventricle prematurely. This ventricular stimulation is premature because the bypass tract conducts rapidly, like most myocardial tissue. Thus, an impulse traveling over the bypass tract does not display the delay seen when an impulse encounters the AV node. Preexcitation is usually manifested by a short PR interval and a slurring of the onset of the QRS complex (which is termed a delta wave). In patients whose bypass tracts are capable of antegrade conduction, most QRS complexes are actually fusion beats between ventricular stimulation via the normal AV conduction system and ventricular stimulation via the bypass tract. The degree of preexcitation then depends on several factors, including the AV nodal conduction time (the slower AV nodal conduction, the larger the delta wave);

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Fig. 6.18 Preexcitation. In this example, there is a left-sided AV bypass tract. An impulse arising from the SA node stimulates the ventricles via both the normal conducting system and the bypass tract. Thus, the resulting QRS complex represents a fusion beat between normal and eccentric activation. Because conduction through the bypass tract does not display the normal conduction delay seen in the AV node, earliest ventricular activation classically occurs via the bypass tract. Hence, the PR interval is shorter than normal, and the QRS complex has a slurred onset known as a delta wave (thick arrow). Patients whose bypass tracts conduct antegradely as shown are said to have Wolff-Parkinson-White syndrome.

Fig. 6.19 A typical 12-lead ECG from a patient with an AV bypass tract. Note the short PR interval and the delta wave visible on most leads.

the conduction velocity and the refractory period of the bypass tract itself (more preexcitation occurs in tracts with rapid conduction velocity and shorter refractory periods); and the proximity of the bypass tract to the SA node (the atrial impulse reaches a right-sided bypass tract

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earlier than it reaches a left-sided bypass tract, and thus right-sided bypass tracts tend to preexcite more). In many patients who present with supraventricular tachycardia mediated by bypass tracts, the bypass tracts are incapable of antegrade conduction. Instead, they conduct in the retrograde direction only. Such bypass tracts are called concealed bypass tracts, because they never manifest delta waves or short PR intervals and are totally inapparent on the ECG when the patient is in normal sinus rhythm. Bypass tracts are clinically signiﬁcant for three reasons. First, they can confuse the clinician. Delta waves can masquerade as Q waves and lead to the false diagnosis of myocardial infarction. Marked preexcitation that occurs during an atrial tachycardia can lead to the mistaken diagnosis of ventricular tachycardia. Second, bypass tracts often act as one pathway of a macroreentrant circuit (the normal AV conduction system acting as the second pathway). Thus, macroreentrant supraventricular tachycardia is common in patients with bypass tracts. Third, bypass tracts can bypass the normal protective mechanism of the AV node during atrial tachyarrhythmias (speciﬁcally, during atrial ﬂutter or ﬁbrillation). In bypass tracts with short antegrade refractory periods, extremely rapid ventricular rates can result during atrial tachyarrhythmias. This problem is life-threatening. The electrophysiology study can play a major role in characterizing the signiﬁcance of bypass tracts and developing appropriate therapy. The electrophysiology study can be used to determine the characteristics of the pathways of a macroreentrant circuit and can help to select effective therapy for macroreentrant arrhythmias. In addition, the electrophysiology study can help to determine the potential of the bypass tract to mediate lethal arrhythmias (the potential for lethal arrhythmias is not an issue in patients with concealed bypass tracts, since it depends on efﬁcient antegrade conduction). Finally, and most importantly, the electrophysiology study can be used to precisely localize and ablate the bypass tract (see Chapter 8). Indeed, rare is the electrophysiologist today who identiﬁes a bypass tract without ablating it. The electrophysiology study in bypass tract-mediated macroreentry The mechanism of macroreentrant supraventricular tachycardia

Macroreentrant “supraventricular” tachycardia is actually a misnomer because the reentrant circuit involves ventricular as well as supraventricular structures. The mechanism of this arrhythmia is illustrated in Figure 6.20. A bypass tract acts as one of the pathways of the reentrant

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Fig. 6.20 Bypass tract-mediated macroreentry. In this illustration, a left-sided AV bypass tract is present. (A) A normal impulse arising in the SA node stimulates the ventricle via both the normal conducting system and the bypass tract, as in Fig. 6.18. The resulting ECG shows the typical short PR interval and delta wave. (B) A premature atrial complex occurs during the refractory period of the bypass tract (which typically has a longer refractory period than the AV node). The impulse thus blocks in the bypass tract and reaches the ventricle solely via the normal conducting pathway, and with a normal PR interval (depending on the site of origin of the premature atrial contraction [PAC]) and a normal (i.e., no delta wave) QRS complex. (C) Because the PAC has blocked antegradely in the bypass tract, the bypass tract may no longer be refractory by the time the impulse reaches the ventricles by way of the normal conducting system. In this case, the bypass tract may be able to conduct the impulse retrogradely back to the atrium. Thus, a reentrant impulse is established, which travels antegradely down the normal conducting system and retrogradely up the bypass tract. This form of macroreentry is extremely common in patients with AV bypass tracts.

circuit. Like pathway B in our model of reentry, the bypass tract conducts rapidly, and often has a relatively long refractory period. The pathway A of the reentrant circuit is formed by the normal AV conduction system, which displays the characteristics of slow conduction and a relatively short ERP. In short, in a heart containing a bypass tract, the characteristics of an ideal reentrant circuit are often present (Figure 6.20A). A macroreentrant rhythm can then often be started simply by introducing an atrial premature impulse at a time when the bypass tract is still refractory from the previous impulse but when the AV node has recovered (Figures 6.20B and 6.20C). The macroreentrant tachycardia has a normal QRS complex because antegrade conduction is via the normal AV conduction system.

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Mode of initiation and termination of macroreentry

Bypass tract-mediated macroreentrant supraventricular tachyarrhythmias can usually be both initiated and terminated with either atrial or ventricular pacing. In the presence of a bypass tract, macroreentry is often inducible with a single atrial extrastimulus. In the case of a bypass tract that is capable of antegrade conduction, a typical response to a series of single premature atrial impulses with progressively shorter cycle lengths is shown in Figure 6.21. Premature impulses with relatively long coupling intervals may show only moderate preexcitation (Figure 6.21A). As coupling intervals are shortened, conduction in the AV node is prolonged, so that the resultant QRS complexes show progressively more preexcitation (i.e., impulses have more time to depolarize the ventricles via the bypass tract [Figure 6.21B]). When the coupling interval is shorter than the ERP of the bypass tract, the impulse suddenly blocks in the bypass tract and conducts entirely via the normal AV conduction system. The resultant QRS complex shows no preexcitation (Figure 6.21C). If conduction of this impulse through the normal AV conduction system is slow enough, the bypass tract may have enough time to recover so that the impulse may conduct retrogradely back to the atria, thus initiating macroreentry. The conduction delay seen with the onset of macroreentrant tachycardia represents the shift in AV conduction from the bypass tract to the AV node. The beginning of the tachycardia zone in macroreentry is thus related to the ERP of the bypass tract. In general, with even earlier premature atrial stimuli, macroreentry will be reproducibly inducible until the ERP of the AV conduction system is reached (the end of the tachycardia zone). In the case of concealed bypass tracts (which are not capable of antegrade conduction), the initiation of macroreentry is somewhat more difﬁcult to visualize. If there was truly no antegrade conduction down the bypass tract, one would expect every normally conducted sinus beat to conduct retrogradely back up the bypass tract and thus to initiate reentry. Because this is not the case, sinus beats must partially penetrate the bypass tract in the antegrade direction, rendering it refractory to subsequent retrograde conduction (Figure 6.22). (This phenomenon of conduction into a structure that cannot be directly observed but that one can deduce because of its effect on subsequent refractoriness is called concealed conduction.) To initiate macroreentry with atrial extrastimuli in patients with a concealed bypass tract, the extrastimulus must occur early enough so that concealed conduction into the bypass tract is blocked (i.e., the extrastimulus must occur during the antegrade ERP of the concealed bypass tract [Figure 6.22]).

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Fig. 6.21 Initiation of macroreentry. This ﬁgure shows the induction of macroreentry with a single extrastimulus from the right atrium (i.e., by the mechanism illustrated in Fig. 6.20). A surface ECG lead and the His bundle electrogram are depicted. (A) At a relatively long S1–S2 coupling interval, the premature atrial impulse conducts down both the normal conducting system and the bypass tract. The resultant QRS complex resembles the QRS complex in sinus rhythm (the last complex in [A]). (B) A premature atrial impulse with a shorter coupling interval encounters more delay in the AV node than was present in (A). Thus, the resultant QRS complex shows more preexcitation (more of the ventricle is depolarized via the bypass tract, while the impulse slowly wends its way through the AV node). The H spike is not visible during the premature beat in (B) because the His bundle is not stimulated until well into ventricular depolarization. (C) An even earlier atrial premature beat now encounters the refractory period of the bypass tract. Thus, the premature impulse reaches the ventricles entirely through the normal conducting system. Note the relatively long AH interval following the S2 impulse, and the narrow (nonpreexcited) QRS complex. The impulse then returns to the atria retrogradely via the bypass tract, and macroreentrant tachycardia is established.

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Fig. 6.22 Initiation of macroreentry with a concealed bypass tract. With concealed bypass tracts, no atrial impulses are capable of reaching the ventricles via the bypass tract. However, some antegrade penetration of the bypass tract must be occurring, otherwise every atrial impulse would initiate reentry. This hidden conduction into the concealed bypass tract (called concealed penetration) is depicted in the ﬁrst panel. Concealed antegrade penetration renders the bypass tract refractory to retrograde conduction and prevents reentry. Note that with a concealed bypass tract, the PR interval is normal and there is no delta wave. In the second panel, a premature atrial impulse occurs during the refractory period of the bypass tract, preventing concealed penetration from occurring. Because the bypass tract is not stimulated in the antegrade direction, the impulse may now conduct retrogradely back up the bypass tract and thus initiate reentry.

In addition, the extrastimulus must occur early enough to cause sufﬁcient delay in AV conduction so that the bypass tract has time to recover from concealed conduction. Induction of macroreentry in patients with concealed bypass tracts is facilitated by pacing near the bypass tract. Concealed conduction into the bypass tract then occurs early, and the bypass tract has more time to recover for subsequent retrograde conduction. With either typical or concealed bypass tracts, macroreentry can also be induced with incremental atrial pacing, as long as pacing is rapid enough to cause complete or intermittent antegrade block in the bypass tract.

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As opposed to AV nodal reentry, bypass tract-mediated macroreentry is often easy to induce with ventricular pacing. This is because retrograde conduction via the normal AV conduction system is often inefﬁcient and therefore quick to block. Ventricular impuses that block retrogradely in the His bundle but conduct up the bypass tract will often induce reentry. Termination of macroreentrant tachycardia can be accomplished with either atrial or ventricular extrastimuli. Atrial premature beats generally terminate macroreentry by occurring early enough to block antegradely in the AV node. Likewise, ventricular premature beats terminate macroreentry most commonly by preexciting the atrium (retrogradely via the bypass tract) early enough to produce antegrade block in the AV node. Patterns of atrial and ventricular activation in bypass tract-mediated reentry

In bypass tracts that are capable of antegrade conduction, the ventricular activation patterns in sinus rhythm or with premature atrial complexes will be abnormal to the extent that preexcitation occurs. If one could record intracardiac electrograms along the ventricular side of the AV groove, the earliest ventricular activation would be seen at the ventricular insertion of the bypass tract. Because bypass tracts usually conduct rapidly and with constant conduction times until block occurs, the AV interval (or the PR interval) remains relatively constant with progressively premature atrial impulses until the ERP of the bypass tract is reached. The AV conduction curve is thus ﬂat until block in the bypass tract occurs and AV conduction shifts to the AV node (Figure 6.23). In patients with concealed bypass tracts, no preexcitation is seen. In these patients, the AV conduction curve is normal, unless there are concomitant and unrelated dual AV nodal pathways. Retrograde activation of the atrium is abnormal in patients who have left-sided or right-sided bypass tracts (see Figure 6.10). Often, with ventricular paced beats that have relatively long coupling intervals, atrial fusion occurs between normally conducted retrograde impulses and impulses that conduct up the bypass tract. With shorter coupling intervals, conduction up the normal pathways is delayed or blocked, and retrograde activation patterns are frankly abnormal. In patients who have anterior septal bypass tracts, the retrograde activation pattern of the atrium appears normal because the atrial insertion of these tracts is near the AV node. In these patients, however, progressively earlier ventricular paced beats do not result in a progressive delay in retrograde conduction time, as one would expect to see in

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Fig. 6.23 A typical AV conduction curve in a patient with an AV bypass tract. At longer coupling intervals, premature atrial impulses are conducted to the ventricles via the bypass tract. Because the bypass tract does not typically display slowing in conduction with premature beats, this portion of the curve is ﬂat. When the refractory period of the bypass tract is reached, AV conduction shifts to the normal AV conducting system. Thus, the curve is discontinuous. At the point where the curve shifts, the delta wave disappears from the resulting QRS complex. Also at this point, macroreentry is likely to occur. Intracardiac electrograms displaying this phenomenon are shown in Fig. 6.21.

retrograde conduction via the normal AV conduction system. The normal delay in retrograde atrial activation with progressively earlier ventricular stimulation is shown in Figures 6.8 and 6.9. Requirement of the atria and ventricles in macroreentry

The reentrant circuit in macroreentrant tachycardia includes atrial and ventricular myocardium. Any instance of antegrade or retrograde block occurring during the tachycardia, without producing a change in the tachycardia, rules out macroreentry, because a single blocked impulse in either direction should immediately terminate the arrhythmia. During tachycardia, premature atrial or ventricular extrastimuli can readily reset the tachycardia — this phenomenon can be used as evidence that the atria and ventricles are part of the circuit. An appropriately timed premature ventricular stimulus during tachycardia can often be shown to preexcite the atrium, which is strong evidence that retrograde stimulation via a bypass tract is operational (Figure 6.24). During

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Fig. 6.24 Atrial preexcitation during macroreentry. A surface ECG lead and intracardiac electrograms from the high right atrium (HRA), His bundle, coronary sinus (CS), and right ventricular apex (RVA) are shown. Macroreentrant tachycardia is present with a cycle length of 360 msec. During the tachycardia, a single extrastimulus is delivered to the RVA at a coupling interval of 290 msec (arrow). This ventricular stimulation results in a premature retrograde atrial impulse at the same coupling interval (290 msec), best seen in the HRA electrogram. Preexcitation of the atrium with ventricular pacing during supraventricular tachycardia is strong evidence that an AV bypass tract is present.

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macroreentry, the development of bundle branch block on the same side of the heart as the bypass tract will increase the cycle length of the tachycardia, strongly suggesting that the ventricles are part of the circuit (see Figure 6.11). Relationship of the P to QRS during macroreentrant tachycardia

As opposed to AV nodal reentry, in which the atria and ventricles are being depolarized nearly simultaneously, in macroreentry, the atria and the ventricles are being depolarized sequentially. Thus, distinct P waves are virtually always seen. P waves tend to be less than halfway between successive QRS complexes (the RP interval is shorter than the PR interval) because retrograde conduction via the bypass tract tends to be faster than antegrade conduction via the normal AV conducting system (Figure 6.25). Because atrial stimulation is in the retrograde direction, the P wave axis is superior — the P waves will be negative in the inferior leads (II, III, and AVF). Treatment of macroreentrant supraventricular tachycardia

The main goal of pharmacologic therapy in macroreentry is to reduce the width of the tachycardia zone. Drugs that increase the refractory period of the AV node (digitalis, calcium blockers, and β blockers) can decrease the width of the tachycardia zone. In practice, however, the best results are often obtained not so much by narrowing the tachycardia zone as by increasing AV nodal block, thus resulting in Wenckebach conduction whenever tachycardia begins. This is effective therapy because a single blocked beat immediately terminates the tachycardia.

Fig. 6.25 Macroreentrant tachycardia. Three surface EGG leads are shown, but P waves are best seen on the bottom tracing. The PR interval is typically longer than the RP interval.

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Another approach is to attempt to increase the retrograde refractory period of the bypass tract with class Ia drugs. Unfortunately, class Ia drugs also usually increase the antegrade refractory period of the bypass tract, which has the effect of increasing the tachycardia zone. Thus, class Ia drugs tend to be beneﬁcial only when they have an extreme effect on the bypass tract, achieving “pharmacological ablation”. If the effect of the drug is only moderate, macroreentry is often potentiated. In general, the best results with drug therapy are obtained by using drugs that affect AV nodal conduction and refractoriness, either alone or in combination with class Ia drugs. Class Ic drugs such as ﬂecainide and propafenone are often effective in treating macroreentrant tachycardia. Amiodarone is likewise effective, but most electrophysiologists consider it potentially too toxic to use in patients with nonlethal arrhythmias. Antitachycardia pacemakers have been used successfully in patients with macroreentrant tachycardias because these arrhythmias are almost always terminable by programmed pacing. Today, however, all of these alternatives are considered suboptimal, since most bypass tracts can be ablated in the electrophysiology laboratory with a high degree of success. Localization of bypass tracts

Deﬁning the location of bypass tracts is important if transcatheter ablation of the tract is contemplated. As noted, bypass tracts can occur anywhere along the AV groove (except in the space between the aortic and mitral valves). The classiﬁcation of bypass tracts as type A (positive QRS in lead V1) or type B (negative QRS in lead V1) is outmoded and of little use for localizing bypass tracts. Currently, AV bypass tracts are thought of as occurring in one of ﬁve general locations: The left free wall, the right free wall, the posterior septum, the anterior septum, and the midseptum. Deﬁning the location of a bypass tract is accomplished by studying the 12-lead ECG and by intracardiac mapping in the electrophysiology laboratory. The location of bypass tracts as determined by intracardiac mapping has been correlated with the ﬁndings on the 12-lead ECG. The ECG patterns that have emerged match reasonably well with the ﬁve general locations of bypass tracts and are described in Chapter 8. In the electrophysiology laboratory, bypass tracts are localized by studying the patterns of ventricular activation during preexcitation and of atrial activation during retrograde conduction. Left-sided and posterior septal tracts are the easiest to localize. The coronary sinus catheter lies in the AV groove between the left atrium and the left ventricle, and

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the os of the coronary sinus lies in the posterior septal region. By recording electrograms from multiple electrode pairs from an electrode catheter in the coronary sinus, early activation of the left atrium during retrograde conduction (and of the left ventricle during preexcitation) can be precisely localized. Right free wall and anterior septal tracts are more difﬁcult to localize precisely because there is no structure analogous to the coronary sinus that allows mapping of the right AV groove. Nonetheless, in the past few years, electrophysiologists have become quite adept at precisely localizing bypass tracts. See Chapter 8 for details. Atrial ﬂutter/ﬁbrillation in patients with bypass tracts

For reasons that are not well understood, patients with bypass tracts seem more predisposed to developing atrial ﬂutter and ﬁbrillation than the general population is. Because some bypass tracts have the propensity for rapid conduction, an exceedingly rapid ventricular response can be seen in the presence of these arrhythmias (obviously, this is not a problem in patients with concealed bypass tracts). Patients who have rapidly conducting bypass tracts with short antegrade refractory periods are capable of conducting in excess of 300 beats/min (Figure 6.26). Thus, when performing electrophysiologic testing in patients with bypass tracts, it is important to assess the antegrade refractory period and the conduction velocity of the bypass tract during atrial ﬁbrillation. During the electrophysiology study, the refractory periods of the bypass tract are measured in sinus rhythm and with atrial pacing. It is important to keep in mind, however, that bypass tracts respond to rapid stimulation like atrial or ventricular myocardium and not like AV nodal tissue — the faster the tract is stimulated, the shorter is its refractory periods and the faster is its conduction. Thus, the only way to know for

Fig. 6.26 Atrial ﬁbrillation in a patient with an AV bypass tract. Some patients with AV bypass tracts may experience extremely rapid conduction down the bypass tract during atrial tachyarrhythmias. The resulting QRS complexes are wide because ventricular stimulation is almost entirely via the bypass tract. This is a life-threatening arrhythmia.

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sure how fast the tract can conduct during atrial ﬁbrillation or atrial ﬂutter is to attempt to induce these arrhythmias during the study. Further, because bypass tracts tend to respond somewhat to sympathetic stimulation, it is best to test the effect of atrial ﬁbrillation on the bypass tract during an isoproterenol infusion. In general, bypass tracts are considered to be benign when the shortest preexcited RR interval during atrial ﬁbrillation is greater than 270 msec. If the RR intervals are shorter than this, most electrophysiologists feel compelled to administer therapy. Until relatively recently, the most common treatment for potentially lethal bypass tracts was to administer drugs to increase the antegrade refractory period of the bypass tract, such as drugs in class Ia, Ic, or III. After administration of these drugs, their effect must be tested by reinducing atrial ﬁbrillation/ﬂutter. Quite commonly, such pharmacologic therapy appears effective until isoproterenol is again infused, at which time the beneﬁt of the antiarrhythmic drug is often counteracted. In these instances, the addition of a β blocker is often helpful. In patients who have potentially lethal bypass tracts, the addition of a class Ia drug, by increasing the antegrade ERP of the bypass tract and thus widening the tachycardia zone, can make macroreentry much more likely to occur. In these patients, the addition of a drug that affects the AV node can often be of beneﬁt (using a β blocker in this instance can both reduce macroreentry and counter the effect of sympathetic stimulation on the antegrade ERP of the bypass tract). Some drugs, particularly digitalis and verapamil, can actually reduce the antegrade ERP of bypass tracts, rendering the tracts more dangerous. These drugs should generally be avoided in patients with preexcitation. If they are to be used, their effect on the antegrade ERP of the bypass tract should be speciﬁcally measured in the electrophysiology laboratory. Given all the drawbacks to using chronic antiarrhythmic drug therapy in patients with potentially malignant bypass tracts, the treatment of choice for most of these patients is radiofrequency ablation of the bypass tract. Not only does ablation eliminate the bypass tract, but it also eliminates the necessity of taking chronic daily antiarrhythmic drug therapy. This factor is especially important considering that the majority of patients presenting with bypass tracts are relatively young. Uncommon varieties of bypass tracts AV nodal bypass tracts

AV nodal bypass tracts (tract B in Figure 6.17) are relatively rare bypass tracts that connect the low septal atrium to the distal conducting system

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(usually to the His bundle), thus bypassing the AV node. On the surface ECG, patients with AV nodal bypass tracts display a short PR interval and a normal QRS complex. The His electrogram in a patient with such a bypass tract reveals a short AH interval. These bypass tracts display the same electrophysiologic characteristics as the bypass tracts we have been discussing; that is, they behave like myocardial tissue rather than like AV nodal tissue. Although patients with AV nodal bypass tracts can occasionally have reentrant arrhythmias using the bypass tract as the retrograde pathway and the normal AV node as the antegrade pathway, the major clinical problem with these tracts is their propensity to conduct impulses to the ventricle extremely rapidly during atrial ﬁbrillation. Drug therapy to prevent rapid conduction during atrial tachyarrhythmias consists of class Ia or Ic drugs because these tracts do not respond to the usual AV nodal blocking agents, but again, ablation of these tracts is generally the treatment of choice. Mahaim bypass tracts

Mahaim bypass tracts (see Figure 6.17, tract C) form connections between atrial muscle and the right bundle branch (atriofascicular tracts) or between atrial muscle and ventricular muscle (atrioventricular ﬁbers). These tracts, which are discussed in more detail in Chapter 8, do not have typical bypass tract electrophysiology but instead display the kind of decremental conduction seen in AV nodal tissue. Reentrant tachycardia, when it occurs with Mahaim tracts, uses the bypass tract in the antegrade direction and the normal conducting system in the retrograde direction. Since right bundle branch preexcitation occurs in tachycardia mediated by these tracts, the tachycardia displays a left bundle branch block conﬁguration. Fasiculoventricular bypass tracts

These tracts (tract D in Figure 6.17) connect the His bundle or the Purkinje ﬁbers to ventricular myocardium. They are extremely rare and, because they almost never mediate reentrant arrhythmias, they have little clinical signiﬁcance. Their only manifestation is a short HV interval. Multiple bypass tracts

Approximately 10% of patients with bypass tracts have more than one bypass tract. Multiple bypass tracts, when present, can be difﬁcult to diagnose in the electrophysiology laboratory, because one bypass tract almost always predominates and prevents other tracts from

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manifesting themselves. Additional tracts become clinically signiﬁcant most often following ablation of a bypass tract — successful ablation of the target bypass tract allows the hidden tract to become apparent. Multiple bypass tracts are more likely to be present if the 12-lead ECG shows atypical delta waves (including delta waves that appear to shift axis over time) or preexcited tachycardias. Multiple tracts are also likely if either multiple routes of atrial activation or mismatch of antegrade and retrograde activation during macroreentrant tachycardia is seen during electrophysiologic testing. Surgical treatment of bypass tracts

During the mid- to late 1980s, surgical disruption of bypass tracts became an attractive therapeutic option for patients whose arrhythmias could not be controlled with pharmacologic regimens. Although surgery to ablate bypass tracts has been almost entirely supplanted by transcatheter ablation techniques, such surgery is still rarely required when catheter techniques have failed. Surgical disruption of bypass tracts is usually performed while the patient is on cardiopulmonary bypass. Generally, a blunt dissection of the portion of the AV groove that contains the bypass tract is performed via an atriotomy. Before surgery, careful electrophysiologic testing is performed to characterize and localize the bypass tract as fully as possible, and mapping is repeated in the operating room before the patient is placed on cardiopulmonary bypass.

The electrophysiology study in intraatrial reentry Intraatrial reentry is the mechanism of arrhythmia in less than 5% of patients presenting with supraventricular tachycardias. In intraatrial reentry, the reentrant circuit is entirely contained within the atrial myocardium. Superﬁcially, intraatrial reentry resembles automatic atrial tachycardia because distinct P waves precede each QRS complex, P wave morphology almost always differs from normal sinus P waves, and AV block can occur without affecting the arrhythmic mechanism. Unlike automatic atrial reentry, however, intraatrial reentry is inducible and terminable with pacing. Induction of intraatrial reentry is accomplished with atrial pacing. Invariably, whether the arrhythmia is induced with a single extrastimulus or with incremental atrial extrastimuli, induction occurs only when a premature impulse is early enough to produce intraatrial conduction delay (i.e., during the RRP of the atrium). The requirement

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for intraatrial conduction delay is further evidence that the arrhythmia being induced is reentrant in mechanism and that the atrial myocardium forms at least part of the reentrant circuit. During intraatrial reentry, the atrial activation pattern differs from the normal atrial activation pattern because the atria are usually activated from a different location than during sinus rhythm. If the site of intraatrial reentry is near the SA node, however, the activation pattern can be indistinguishable from normal. In these cases, intraatrial reentry can often be distinguished from SA nodal reentry by the necessity of intraatrial conduction delay for initiation of the arrhythmia. Because intraatrial reentrant circuits are contained entirely in atrial tissue, AV nodal block or block in the more distal conducting system can often be observed to occur without affecting the reentrant mechanism, thus demonstrating that the arrhythmia does not require the ventricular myocardium. The pharmacologic treatment of intraatrial reentry requires drugs that affect the atrial myocardium; namely, antiarrhythmic drugs in classes Ia, Ic and III. Drugs that affect primarily the AV node do not affect this arrhythmia (except perhaps to induce heart block). Antitachycardia pacemakers have occasionally been used to terminate intraatrial reentry. Transcatheter ablation of intraatrial reentry, using radiofrequency energy, has also been performed. This procedure, however, tends to be more difﬁcult than the transcatheter ablation of slow AV nodal pathways or of bypass tracts.

The electrophysiology study in SA nodal reentry Sinoatrial nodal reentry is a rare form of reentrant supraventricular tachycardia in which the reentrant circuit is enclosed entirely within the SA node. Because SA nodal tissue is electrophysiologically similar to AV nodal tissue, the mechanism of SA nodal reentry is felt to be the same as that of AV nodal reentry. Most likely, there are dual tracts within the SA node that form a potential reentrant circuit. The P wave morphology on the surface ECG and the atrial activation pattern during SA nodal reentry are normal. SA nodal reentry is distinguished from standard sinus tachycardia by its paroxysmal onset and termination and by the ability to induce and terminate the arrhythmia by pacing. Inducing and terminating SA nodal reentry is possible with atrial pacing, using either single extrastimuli or incremental pacing. Unlike in intraatrial reentry, conduction delay within the atrial myocardium is not necessary for the induction of SA nodal reentry. It is likely that

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the conduction delay necessary for the initiation of reentry occurs in a reentrant circuit enclosed within the SA node, where it cannot be demonstrated. Treatment of SA nodal reentry is similar to the treatment of AV nodal reentry. This arrhythmia responds to vagal maneuvers and to drugs that decrease conduction and increase refractoriness in the SA and AV nodes (digitalis, calcium blockers, and β blockers). SA nodal ablation can also be performed, but a permanent pacemaker may be required as a consequence.

The electrophysiology study in atrial ﬂutter and atrial ﬁbrillation Atrial ﬂutter and atrial ﬁbrillation are felt to be reentrant supraventricular tachyarrhythmias in which the reentrant circuits are located entirely within the atrial myocardium. Both are inducible with single atrial extrastimuli or incremental atrial pacing during the atrial relative refractory period (RRP; i.e., during pacing with coupling intervals short enough to produce intraatrial conduction delay). In atrial ﬂutter, distinct P waves are seen, classically in a sawtooth pattern. In atrial ﬁbrillation, atrial activity is continuous and chaotic, hence distinct P waves are not seen. In both arrhythmias, second-degree AV block is the rule. Atrial ﬂutter

Patients who have paroxysms of atrial ﬂutter often have normal hearts, whereas patients with chronic atrial ﬂutter usually have underlying heart disease that causes atrial distention or dilation. Most often, chronic atrial ﬂutter eventually converts to chronic atrial ﬁbrillation. Patients in whom atrial ﬂutter is inducible during electrophysiologic testing tend to have demonstrable intraatrial conduction abnormalities. In these patients, atrial ﬂutter is usually induced with atrial pacing at cycle lengths that are short enough to produce intraatrial conduction delays. As already noted, these same characteristics are also typical for intraatrial reentrant tachycardias. It is probably legitimate to think of intraatrial reentry, atrial ﬂutter, and atrial ﬁbrillation as forming a spectrum of arrhythmias that have the same essential mechanism — that is, intraatrial reentry. Atrial ﬂutter is distinguished from intraatrial reentrant tachycardia by its rate (ﬂutter occurs from 220 to 350 beats/min, whereas intraatrial reentrant tachycardia occurs from 120 to 220 beats/ min) and by its mode of termination. Whereas intraatrial reentrant

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tachycardia can often be terminated with single programmed atrial premature impulses, atrial ﬂutter cannot. Atrial ﬂutter generally requires rapid atrial pacing for several seconds at rates from 20% to 50% faster than the ﬂutter rate to terminate the arrhythmia. The intraatrial electrogram recorded during atrial ﬂutter normally shows rapid regular deﬂections with uniform cycle lengths and amplitude; the deﬂections correlate with the P waves on the surface ECG (Figure 6.27A). If this typical pattern is seen, the atrial ﬂutter can almost always be terminated with rapid atrial pacing. In some cases of ﬂutter, however, the intraatrial electrogram shows variability in the cycle length and amplitude of the atrial deﬂections. This second type of ﬂutter is probably actually a form of atrial ﬁbrillation (Figure 6.27B). When this pattern is seen on the intraatrial electrogram, termination of the arrhythmia with rapid atrial pacing is usually not possible. On the

Fig. 6.27 Two types of atrial ﬂutter. A surface ECG lead and a right atrial electrogram are shown in both panels. (A) Typical atrial ﬂutter displays a constant amplitude and cycle length on the intracardiac electrogram. This type of ﬂutter is relatively easy to terminate with pacing. (B) Atypical ﬂutter shows a somewhat variable cycle length and amplitude on the intracardiac electrogram. This type of ﬂutter may be intermediate between atrial ﬂutter and atrial ﬁbrillation and is relatively difﬁcult to terminate with pacing.

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surface ECG, this intermediate form of ﬂutter is often called atrial ﬁbﬂutter because the atrial activity appears ﬂutter-like but somewhat irregular, and the ventricular response is often irregular. When vigorous attempts to pace-terminate the typical form of atrial ﬂutter are made, two basic responses are commonly seen. The rhythm may be converted to sinus rhythm or to atrial ﬁbrillation. Generally, atrial ﬁbrillation is more likely to result when faster pacing rates are used (paced cycle lengths approaching 150% of the atrial ﬂutter cycle length). When atrial ﬁbrillation is the result of pace-termination of atrial ﬂutter, the ﬁbrillation usually spontaneously converts to sinus rhythm within 24 hours. Treatment of atrial ﬂutter

In general, the treatment of atrial ﬂutter consists of restoring and maintaining sinus rhythm. Restoring sinus rhythm is most readily accomplished either by pace-termination of the ﬂutter or by DC cardioversion. If atrial ﬂutter recurs, then chronic therapy to prevent atrial ﬂutter should be considered. Until recently, such chronic suppressive therapy was limited to antiarrhythmic drugs (class Ia, Ic, or III drugs). During the past few years, however, effective transcatheter ablation techniques have been developed for preventing atrial ﬂutter. Transcatheter ablation of this arrhythmia (described in Chapter 8) should be considered for any patient in whom chronic antiarrhythmic drug therapy is being contemplated. Atrial ﬁbrillation

Atrial ﬁbrillation can be paroxysmal (usually associated with normal hearts) or chronic (usually associated with heart disease). Although atrial ﬁbrillation is thought to be a reentrant arrhythmia of the atrial myocardium, its continuous and chaotic atrial activity precludes meaningful analysis by recording intraatrial electrograms and also precludes pace-termination of the arrhythmia. Thus, although atrial ﬁbrillation can be induced by pacing, it cannot be terminated by pacing. During standard electrophysiologic testing of the SA node and AV conduction, a few seconds of atrial ﬁbrillation are induced in 5% of normal patients. The induced atrial ﬁbrillation is likely to terminate spontaneously within seconds, unless the patient has a history of spontaneous atrial ﬁbrillation. Patients with a history of atrial ﬁbrillation have a high incidence of intraatrial conduction defects on electrophysiologic testing, similar to patients who have atrial ﬂutter and intraatrial reentrant tachycardia. In patients with atrial ﬁbrillation, however, the conduction defects tend to

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be more generalized, often involving the SA node and AV conduction system as well. Treatment of atrial ﬁbrillation

Atrial ﬁbrillation is one of the most common cardiac arrhythmias seen in medical practice, so it is unfortunate that it is also one of the most difﬁcult to treat. The difﬁculty stems from the fact that there are no widely applicable, reliable and safe methods for restoring and maintaining sinus rhythm in patients with atrial ﬁbrillation. So, in many instances, the most expedient path is to allow the arrhythmia to persist, while controlling the ventricular rate and anticoagulating. In any case, the fundamental decision that must be made when treating atrial ﬁbrillation is whether to aim for rhythm control or for rate control. Rhythm control

Opting for rhythm control commits the physician to ﬁrst restoring, then trying to maintain sinus rhythm. Restoring sinus rhythm is usually straightforward — the main issue involves the timing of cardioversion, so as to reduce the risk of systemic embolization. If atrial ﬁbrillation is known or suspected to have been present for more than 48 hours, one should assume that atrial thrombi exist and delay the cardioversion until three to four weeks of anticoagulation can be given. If immediate cardioversion is required and the duration of atrial ﬁbrillation is longer than 48 hours (or is unknown), the safety of cardioversion is improved if no atrial thrombi are seen during transesophageal echocardiography. There are two standard methods for restoring sinus rhythm: DC cardioversion and drug therapy. Electrical cardioversion has the advantage of being highly efﬁcacious as well as non-proarrhythmic. If the patient is stable, however, several drugs are available that can be effective in restoring sinus rhythm, including dofetilide, ﬂecainide, ibutilide, and propafenone. The efﬁcacy of these drugs is generally reported to be 30– 60%; because all of them can cause proarrhythmia, patients need to be monitored for at least several hours after the drugs are administered. When restoring sinus rhythm, one should consider the possibility that the patient has diffuse electrical system disease (as many elderly patients with atrial ﬁbrillation do). Especially if the ventricular response is relatively slow in the absence of AV blocking drugs, precautions should be taken to make sure that immediate pacing support is available after cardioversion, if needed. Only 20–30% of patients restored to sinus rhythm will remain free of atrial ﬁbrillation for one year without antiarrhythmic drug therapy.

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This success rate can be increased to around 50% with Class Ia, Ic, or III drugs; though evidence exists that amiodarone may be able to increase this value to 60–70%. Some implantable deﬁbrillators offer atrial deﬁbrillation in addition to standard ventricular therapies. These atrial deﬁbrillators sometimes can be helpful in supporting a rapid-cardioversion maintenance strategy in patients with occasional episodes of atrial ﬁbrillation. These devices can be programmed to deliver a DC shock either automatically, or only in response to a “triggering” signal either from the patient, or from his or her doctor. The shocks delivered by these devices are quite painful and are not substantially more convenient than an external DC cardioversion, unless the doctor is willing to activate the automatic or patient-triggered modes — an uncommon scenario. Perhaps not surprisingly, implanted atrial deﬁbrillators have not gained much traction in clinical practice. Because antiarrhythmic drugs are only modestly effective in maintaining sinus rhythm and can be quite toxic, a major focus of electrophysiologists over the past 20 years has been trying to ﬁgure out how to “cure” atrial ﬁbrillation, using ablation techniques. While signiﬁcant progress has been made, the ablation of atrial ﬁbrillation is still tedious, not completely effective, and a relatively risky procedure and should be offered only to carefully selected patients by experienced electrophysiologists. The ablation of atrial ﬁbrillation will be discussed in Chapter 8. Rate control

If maintaining sinus rhythm in patients with atrial ﬁbrillation was easy and safe, nobody would opt for rate control. The fact that rate control is nevertheless the standard of therapy speaks volumes about the difﬁculty and risks of rhythm control. Controlling the ventricular rate in atrial ﬁbrillation can usually be accomplished by administering drugs that affect AV nodal conduction and refractoriness (digitalis, calcium blockers, and β blockers). Often, all three types of drugs need to be used in combination to achieve adequate rate control. If rate control cannot be achieved by pharmacologic means, there is a more drastic (though effective and relatively safe) method for doing so — ablating the AV conduction system to produce complete heart block, and then inserting a permanent rate-responsive pacemaker. This option virtually guarantees excellent rate control, and in patients whose symptoms are related to persistently high heart rates, it often creates a dramatic improvement in quality of life. This method is discussed in detail in Chapter 8.

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Rhythm control versus rate control

For decades it has been a point of controversy whether patients with atrial ﬁbrillation are best managed with rhythm control or with rate control. Two recent randomized clinical trials — the AFFIRM trial (Wyse et al., N Engl J Med 2002 Dec 5; 347:1825) and the RACE trial (VanGelder et al., N Engl J Med 2002 Dec 5; 347:1834) — showed no beneﬁt to patients with atrial ﬁbrillation assigned to rhythm control (using antiarrhythmic drugs) when compared to patients assigned to rate control. Indeed, in both trials there was a tendency toward better clinical outcomes in the rate control groups; this latter ﬁnding is generally interpreted as yet more evidence of the toxicity of antiarrhythmic drugs. Furthermore, systemic embolization was not reduced in the rhythm control group, so once a patient has had chronic or persistent atrial ﬁbrillation, chronic anticoagulation apparently remains necessary, even if sinus rhythm is successfully restored and maintained. The bottom line: For now, in general, rate control is the generally accepted standard of treatment for patients with chronic or persistent atrial ﬁbrillation. AFFIRM and RACE do not, however, tell the whole story. Consider the following: • Some patients are signiﬁcantly symptomatic when they are in atrial ﬁbrillation, even if their heart rates are controlled. Usually, these patients have relatively “stiff”, non-compliant ventricles (i.e., diastolic dysfunction). Such patients rely heavily on effective atrial contractions, which allow them to maintain the high left ventricular enddiastolic pressures they require while at the same time maintaining relatively normal mean left atrial pressures. With the onset of atrial ﬁbrillation, the only way to maintain these high left ventricular enddiastolic pressures is to immediately and dramatically elevate the mean left atrial pressures, leading to symptoms related to pulmonary congestion. In individuals like this, no matter what the randomized trials may say, maintaining sinus rhythm is imperative. • Patients with normal hearts and occasional episodes of atrial ﬁbrillation almost always feel much better in sinus rhythm. Maintaining sinus rhythm in these patients is often the more favorable approach. These patients were underrepresented in both AFFIRM and RACE. • A recently published sub-study from the AFFIRM trial suggests that patients who actually achieved chronic sinus rhythm (as opposed to patients merely randomized to rhythm control) had improved clinical outcomes (Corley et al., Circulation 2004; 109:1509). • A recent non-randomized study (Hsu et al., N Engl J Med 2004; 351:2373) suggests that in patients with chronic congestive heart

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failure and rate-controlled atrial ﬁbrillation, the successful ablation of atrial ﬁbrillation yields a signiﬁcantly improved quality of life. These considerations emphasize once again that rate control is the standard of therapy not because it is a perfectly adequate treatment, but because the alternatives are so unappealing. The lack of beneﬁt from rhythm control seen in randomized trials seems most likely to be an artifact of our current ineffective and risky methods for maintaining sinus rhythm. With the further reﬁnement and generalized ability of techniques for ablating atrial ﬁbrillation, this equation will likely change drastically. Nonetheless, in general, rate control now ought to be the predominant treatment strategy used in patients with chronic or persistent atrial ﬁbrillation. For patients with paroxysmal or recent onset atrial ﬁbrillation — in other words, patients who do not have chronic or persistent atrial ﬁbrillation — virtually all experts agree that restoring sinus rhythm is still the best course of action, though not many are enthusiastic about using antiarrhythmic drugs to maintain sinus rhythm even in these patients. Patients with frequent episodes of paroxysmal atrial ﬁbrillation — whose arrhythmias are now thought to be often triggered by ectopic foci located in the pulmonary veins — are probably those who stand to beneﬁt the most from ablation techniques centered around the electrical isolation of the pulmonary veins (See Chapter 8.)

Evaluation of patients with supraventricular tachyarrhythmias — when is electrophysiologic testing necessary? Although the study of supraventricular tachyarrhythmias is probably the most intellectually stimulating and satisfying type of electrophysiology study one can perform, the fact is that many patients with supraventricular tachycardias can be managed adequately without invasive testing. Electrophysiology studies are often not necessary for two reasons. First, if one understands the mechanisms of supraventricular tachyarrhythmias, the astute clinician can often diagnose and treat the arrhythmia based on examination of the surface ECG and on the response to vagal maneuvers. Second, in most cases, supraventricular tachyarrhythmias are not life-threatening. Therefore, if one guesses incorrectly on therapy, the patient will survive, and one will have an opportunity to change the recommended treatment. (The major exception to this rule is in patients with bypass tracts that have very short antegrade refractory periods.)

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The examination of the surface ECG can help immensely in diagnosing the mechanism of supraventricular tachycardia. Atrial ﬂutter and atrial ﬁbrillation can be diagnosed almost immediately from the ECG and do not present a diagnostic problem. In the other types of supraventricular tachycardias, the relationship of P waves to QRS complexes and the morphology of P waves during tachycardia can be most helpful. Figure 6.28 shows the essential characteristics of the P waves in the four types of reentry that are commonly lumped under the heading PAT. In the majority of patients with AV nodal reentry (the most common form of PAT), the retrograde P waves occur during the QRS complex and are therefore invisible on the 12-lead ECG. In every other kind of PAT, P waves can usually be identiﬁed on careful inspection of the ECG. Therefore, if there are no P waves, AV nodal reentry is the likely diagnosis. In bypass tract-mediated macroreentry (the next most common type of PAT — approximately 90% of patients presenting with PAT have either this or AV nodal reentry), P waves virtually always can be seen. Because the P waves are generated retrogradely during this tachycardia, they are always negative in the inferior leads. Generally, the RP interval is less than the PR interval. Because the RP interval is relatively short, the retrograde P wave is often mistaken for a bump on the T wave by the unwary observer. In intraatrial reentry, P waves are invariably seen on the 12-lead ECG. The PR interval is usually shorter than the RP interval and therefore the P waves are more obvious than in macroreentry. The P wave morphology is quite variable from patient to patient and depends entirely on the location of the reentrant circuit within the atrium. In SA nodal reentry, the P–QRS morphology is almost exactly identical to that seen in normal sinus rhythm. Thus, this arrhythmia is much more likely to be mistaken for sinus tachycardia than any of the other forms of reentrant supraventricular tachycardias. Vagal maneuvers are also helpful in resolving these arrhythmias. Increased vagal tone commonly either decreases the rate of or terminates AV nodal reentry and macroreentry, because the AV node is part of the reentrant circuit in both of these arrhythmias. Likewise, vagal maneuvers may slow or terminate SA nodal reentry. In intraatrial reentry, however, vagal maneuvers have no effect on the cycle length of the tachycardia, but they may prolong the PR interval or produce AV block without changing the tachycardia. Most of the time, the correct mechanism of PAT can be deduced by these noninvasive considerations. Appropriate therapy can then be

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Fig. 6.28 Typical P wave relationships in four types of supraventricular tachycardia. Surface ECG lead II is depicted. (A) In AV nodal reentrant tachycardia, the P wave is usually buried within the QRS complex and is not discernible. (B) In bypass tractmediated macroreentry, the inferior leads usually show a negative P wave, with the RP interval shorter than the PR interval. (C) In intraatrial reentry, discrete P waves are almost always seen. The P wave morphology can have any conﬁguration, and the PR interval is normal or short. (D) In SA nodal reentry, P waves and the PR interval appear normal.

instituted immediately. For instance, when one recognizes that a patient has intraatrial reentry, one can correctly predict that the patient is one of the famous 5% to 10% presenting with PAT who will not respond to intravenous verapamil. Normally, electrophysiologic testing needs to be performed in patients with supraventricular tachyarrhythmias in three general situations. First, electrophysiology studies can be helpful in patients whose arrhythmias appear refractory to treatment. In such patients, the

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arrhythmias usually have not responded to therapy, either because the mechanism of the arrhythmia is unknown or misunderstood, or because the reentrant circuit has unusual characteristics and does not respond to treatment in the usual way. Invasive studies can help immeasurably by identifying the exact mechanism of the arrhythmias and by fully characterizing the various portions of the reentrant circuit. Pharmacologic or nonpharmacologic therapy can then be chosen based on that information. Second, electrophysiology studies are indicated in patients with bypass tracts that are suspected to be capable of mediating life-threatening arrhythmias. Certainly such patients would include those who have already demonstrated the propensity of the bypass tract to conduct dangerously rapidly during atrial ﬁbrillation or ﬂutter. Many electrophysiologists advocate invasive studies in any patient with a bypass tract who has had symptomatic arrhythmias of any type. Some even recommend studying any patient who is seen to have preexcitation on an ECG, on the premise that any bypass tract that conducts antegradely may have lethal potential until proven otherwise. Third, electrophysiology studies are done for the purpose of performing transcatheter ablation. With the remarkable success of transcatheter ablation using radiofrequency energy over the past few years for most varieties of supraventricular tachycardia, it is now advisable to refer any patient for electrophysiologic testing who would otherwise be subjected to daily long-term pharmacologic therapy.

CHAPTER 7

The Electrophysiology Study in the Evaluation and Treatment of Ventricular Arrhythmias

Ventricular tachyarrhythmias and sudden death Sudden death (death that is instantaneous and completely unexpected) may well be the major public health problem in the United States today. If this statement seems surprising, consider that each year, approximately 400,000 Americans die suddenly, and that sudden death is the most common form of death in the United States. Although most Americans are touched by sudden death, few realize that the majority of these deaths are due to electrical disturbances of the heart and are therefore, at least in theory, preventable. Consider a typical sudden cardiac death: A 59-year-old man who has suffered a myocardial infarction within the past 12 months has recovered, is now feeling well, and is leading a happy and productive life. He has followed his physician’s advice and has altered his life-style in an exemplary fashion — he has stopped smoking, is on a low-fat and lowcholesterol diet, and has joined an exercise program. He is back at work, and his new sense of mortality has resulted in a broader and more tolerant perspective on everyday job-related stresses. In many ways, he feels better than he has in years. Then one day, while watching television with his wife, he gasps softly and slumps over. An ambulance is called, but within minutes he is dead. The grieving widow is told by the emergency room physician (who has never seen the victim before) that her husband has died of a heart attack. Later, the victim’s personal physician is only too quick (often through the honest desire to allay any feelings of guilt among surviving family members) to corroborate the “inevitability” of the event. This scene takes place, on average, almost once every minute in the United States. The tragedy is compounded by a lack of understanding by both the lay public and the medical profession as to the reason for these 158

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sudden deaths. Most often, sudden death is not caused by acute myocardial infarction or bradycardia, as is commonly claimed. Instead, the vast majority of the 400,000 sudden deaths that occur each year in the United States are due to ventricular tachycardia or ventricular ﬁbrillation. To the extent that ventricular tachyarrhythmias can be adequately treated, most of these sudden cardiac deaths can be prevented. During the past two or three decades, remarkable advances have been made in treating ventricular tachycardia and ﬁbrillation, largely thanks to what has been learned in the electrophysiology laboratory. It was the recognition that the great majority of lethal arrhythmias are due to the mechanism of reentry, and that they therefore lend themselves nicely to study in the electrophysiology laboratory, that catalyzed the rapid expansion of electrophysiology centers during the 1980s. The original “Holy Grail” for electrophysiologists was to solve the problem of sudden cardiac death. This goal was pursued for years through the careful study of ventricular tachyarrhythmias in the electrophysiology laboratory. For almost 20 years, electrophysiologists spent much of their time inducing and terminating ventricular arrhythmias, and most especially, trying to identify effective therapy for those arrhythmias by the serial testing of antiarrhythmic drugs. Thankfully, serial drug testing for ventricular arrhythmias now has virtually disappeared from the electrophysiologist’s repertoire. So, in contrast to prior editions of this book, where much space in this chapter was devoted to the technique of, and rationale for, serial drug testing, the author now offers instead a chilling speculation on how future historians of medicine might view these recent times: The reader no doubt will be disturbed to learn that, during the last decades of the 20th century, doctors calling themselves “electrophysiologists” submitted thousands of patients to multiple inductions of cardiac arrest, followed by resuscitations, over periods of days to weeks; and further, that this practice was not only legal, but was represented as being therapeutic, and was accepted — and in some instances honored and admired — by their medical colleagues. It is not recorded what these “electrophysiologists” did to sublimate their proclivities once this “serial drug testing” was no longer considered a legitimate medical practice.

In this chapter, we will review the current management of ventricular tachyarrhythmias — and the role that electrophysiologic testing plays in their evaluation and treatment. This role is clearly very different today than it was in the recent past. Nonetheless, the electrophysiology study can still be helpful in managing patients with ventricular tachyarrhythmias, both in diagnosing their problem, and in devising optimal treat-

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ment. And, despite the smug superiority that (the author fears) may color future historians’ view of the matter, it is what we have learned in the electrophysiology laboratory that enables our treatment of these arrhythmias today and (if we allow ourselves to follow the science) opens a path to substantially reducing the millions of sudden deaths that threaten to occur in the future.

The evaluation of ventricular tachyarrhythmias The mechanisms of ventricular arrhythmias

The appropriate evaluation and treatment of ventricular arrhythmias largely depends on the mechanism of those arrhythmias. Table 7.1 lists the most common ventricular arrhythmias according to their mechanisms. Whatever the mechanism, however, ventricular arrhythmias have similar appearances on the ECG: premature ventricular complexes (PVCs), ventricular tachycardia, or ventricular ﬁbrillation. Figuring out which mechanism is responsible when faced with any of these arrhythmias depends to a great extent on the clinical setting in which the arrhythmia occurs — and sometimes on its characteristics in the electrophysiology laboratory.

Table 7.1 Mechanisms of Ventricular Arrhythmias. Automatic ventricular arrhythmias Premature ventricular complexes Ventricular tachycardia and ﬁbrillation associated with acute medical conditions: Acute myocardial infarction or ischemia Electrolyte and acid–base disturbances, hypoxemia Increased sympathetic tone Reentrant ventricular arrhythmias Premature ventricular complexes Ventricular tachycardia and ﬁbrillation associated with chronic heart disease: Previous myocardial infarction Cardiomyopathy (including bundle branch reentry and ventricular arrhythmias associated with arrhythmogenic right ventricular dysplasia) Triggered activity Pause-dependent triggered activity Catechol-dependent triggered activity Miscellaneous ventricular arrhythmias Idiopathic left ventricular tachycardia Outﬂow tract ventricular tachycardia (repetitive monomorphic ventricular tachycardia) Brugada syndrome

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We will discuss these arrhythmias in the order of their clinical frequency, beginning, of course with reentrant ventricular arrhythmias. Reentrant ventricular arrhythmias

Reentry accounts for the majority of ventricular arrhythmias. Reentrant ventricular arrhythmias are most often associated with chronic underlying heart disease. Reentrant circuits within the ventricles usually do not appear until patients develop some form of heart disease which causes scarring in the ventricular myocardium. Such scarring mainly occurs with ischemic heart disease and the various cardiomyopathies. In ischemic heart disease, reentrant circuits arise during the healing and ventricular remodeling that follow an acute myocardial infarction — usually, the reentrant circuits form in the border zone between the scar tissue and the normal myocardium. In contrast to automatic arrhythmias, in which the typical substrate (such as acute ischemia) is temporary in nature and most often reversible, in the case of reentrant arrhythmias the substrate (i.e., the reentrant circuit) is not temporary but ﬁxed. Once a reentrant circuit is formed, it is always present and can generate a reentrant ventricular tachyarrhythmia at any time and without warning. Thus, the “late” sudden deaths that occur in patients with myocardial infarction (i.e., sudden death occurring at a time between roughly 24 hours to months or even years after the acute infarction) are usually due to reentrant arrhythmias. Reentrant arrhythmias, then, are commonly seen in patients who have a history of cardiac disease but are not acutely ill at the time of the arrhythmia. The vast majority of sudden cardiac deaths in the United States are due to reentrant ventricular tachyarrhythmias. Risk factors for reentrant ventricular arrhythmias

It is relatively straightforward to predict which patients are at risk for reentrant ventricular tachyarrhythmias (and, therefore, at risk for sudden cardiac death), as long as one has an understanding of the pathophysiology of reentrant arrhythmias. A reentrant arrhythmia requires both an anatomic circuit with electrophysiologic properties appropriate for sustaining a reentrant impulse, and an appropriately timed premature impulse to trigger the reentrant arrhythmia. Because reentrant circuits are common only in the setting of myocardial disease, the major risk factor for ventricular reentry is the presence of underlying cardiac disease. As noted, myocardial infarctions and cardiomyopathic diseases are the most common disorders associated with reentrant ventricular arrhythmias. Nonetheless, any cardiac condition that causes even a small amount of ventricular ﬁbrosis can give rise to

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reentrant circuits. Such conditions include myocardial trauma, a myocardial infarction that has been “aborted” by thrombolytic therapy, sub-clinical infarctions associated with bypass surgery, or sub-clinical viral myocarditis. In general, the more extensive the myocardial ﬁbrosis, the higher the likelihood of developing a reentrant circuit. With disease states that cause large ﬁbrotic patches (such as a myocardial infarction), reentrant circuits are reasonably likely to develop. In disease states that cause only microscopic ﬁbrosis, however, the likelihood of reentrant arrhythmias is proportional to the degree of myocardial involvement in the underlying disease process. Once an anatomic circuit exists whose electrophysiologic properties are appropriate for sustaining reentry, an appropriately timed premature impulse is required to trigger the reentrant arrhythmia. Thus, another risk factor for developing reentrant ventricular arrhythmias is ventricular ectopy. Complex ventricular ectopy is generally considered to be present if, on 24-hour Holter monitoring, there are more than 10 PVCs complexes per hour or repetitive forms such as couplets, triplets, or runs of nonsustained ventricular tachycardia. Patients with underlying cardiac disease who have complex ventricular ectopy have a higher risk of sudden death than patients who have the same underlying disease without complex ectopy. Frequent ectopic beats are not, however, a requirement for developing reentrant arrhythmias, since a single PVC (or even a premature atrial complex [PAC]) has the potential to trigger a reentrant ventricular tachyarrhythmia, given the right reentrant circuit. Indeed, a substantial proportion of patients resuscitated from lethal arrhythmias have only negligible ventricular ectopy. It should also be noted that complex ventricular ectopy in patients with normal heart muscles (and who therefore are extremely unlikely to have a reentrant circuit within their ventricles) has never been shown to increase the risk of sudden death. An individual’s risk for sudden cardiac death from a reentrant tachycardia, therefore, is most directly dependent on the presence or absence of underlying myocardial disease and on the extent of that disease. In general, since lower ejection fractions imply more extensive scarring and therefore indicate a higher likelihood that a reentrant circuit is present, the lower the ejection fraction, the higher the probability of sudden death. Most fatal arrhythmias occur in patients who have left ventricular ejection fractions of less than 40%. As we have noted, some degree of ectopy also must be present to trigger the reentrant arrhythmia, but that ectopy does not necessarily have to be very frequent for an arrhythmia to occur. The probability that a reentrant circuit will

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generate an arrhythmia is much more dependent on the characteristics of the circuit itself (e.g., the tachycardia zone of the circuit) than on the frequency of ectopic beats. Many studies have been done to attempt to quantify an individual’s risk of sudden death, and most of these studies have focused on three risk factors: The presence of a prior myocardial infarction, the presence of a depressed left ventricular ejection fraction (arbitrarily, less than 40%), and the presence of complex ventricular ectopy. At the risk of greatly oversimplifying the vast body of literature examining this issue let us make the following generalizations. First, the presence of underlying heart disease is more important in determining risk than the presence of complex ectopy, because underlying heart disease alone increases one’s risk for sudden death, whereas complex ectopy alone does not. Second, having one of these risk factors alone (except for complex ectopy) yields a one-year risk of sudden death that can be grossly estimated at approximately 5%. Third, the risk produced by the presence of more than one of these risk factors appears to be roughly additive (Table 7.2). Thus, the presence of either a previous myocardial infarction or a depressed ejection fraction gives a one-year risk of about 5%. The presence of any two risk factors gives a risk of about 10%, and the presence of all three factors gives a risk of about 15%. Obviously, these values represent only a gross estimate derived from the available literature. The severity of each risk factor is also important. For instance, a large myocardial infarction yields a higher risk than a small infarction, an ejection fraction of 15% yields a higher risk than an ejection fraction of 35%, and the presence of nonsustained ventricular tachycardia yields a higher risk than single PVCs. Thus, a patient with a previous large myocardial infarction with severely depressed ventricular function and long runs of nonsustained ventricular tachycardia will have a one-year risk substantially higher than 15%. Another indicator that is sometimes used to estimate risk of reentrant ventricular arrhythmias is the signal-averaged surface ECG. The signalaveraging process digitizes and processes a series of QRS complexes (usually several hundred) recorded from the body surface. The result is a clean, high-ﬁdelity average QRS complex in which small (lowamplitude) details can be seen that are not visible on a normal ECG. In many patients at risk for lethal arrhythmias, low-amplitude afterpotentials can be seen immediately following the QRS complex (Figure 7.1). In theory, these afterpotentials may represent electrical activity caused by localized slow conduction in one or more reentrant circuits. If so, the signal-averaged ECG may be a method of detecting the presence of reentrant circuits in patients who have underlying cardiac disease

164 II Electrophysioloyg Testing for Cardiac Arrhythmias Table 7.2 Risk Factors and Probabilities of Sudden Cardiac Death. Moderate-risk group Risk factors Previous MI or LV EF < 40% Previous MI + LV EF < 40% or Previous MI + complex ectopy or LV EF < 40% + complex ectopy Previous MI + LV EF < 40% + complex ectopy High-risk group Risk factors Sudden death survivor VT with syncope VT with minimal symptoms

1-year risk of sudden death 50%

10%

15%

1-year risk of sudden death 30%–50% 30%–50% 20%–30%

Values on this table are loosely derived from data reported by the Multicenter Postinfarction Research Group (Bigger et al., Circulation 1984; 69:250) and the Multicenter Investigation of the Limitation of Infarction Size (Mukharji et al., Am J Cardiol 1984; 54:31). MI, myocardial infarction; LV EF, left ventricular ejection fraction; VT, ventricular tachycardia.

Fig. 7.1 Signal-averaged ECG. The ﬁrst panel shows a normal signal-averaged ECG, in which no late potentials are present. The second panel shows an abnormal signalaveraged ECG. The late potentials may indicate areas of slow conduction within the ventricular myocardium, suggesting the presence of a reentrant circuit.

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known to predispose to reentry. When considered with other risk factors as listed in Table 7.2, the prognostic value of the signal-averaged ECG appears to be roughly additive. Thus, for instance, a patient with a depressed ejection fraction, a prior myocardial infarction, complex ectopy, and a positive signal-averaged study would have a one-year risk of sudden death up to 20–30%. The signal-averaged ECG should always be interpreted along with these other risk factors. In summary, patients who have survived a myocardial infarction or who have a depressed left ventricular ejection fraction from any cause are at increased risk for sudden death from reentrant ventricular tachyarrhythmias. The risk increases when the underlying cardiac disease is accompanied by complex ventricular ectopy or a positive signalaveraged ECG. Considering only the fact that each year, between 500,000 and 1,000,000 people suffer myocardial infarctions, the pool of patients at risk for sudden cardiac death is seen to be huge. It is from this very large pool of individuals that most of the 400,000 sudden death victims each year are drawn. Clinical characteristics of reentrant ventricular tachyarrhythmias

The reentrant ventricular tachyarrhythmias take two major forms: Ventricular tachycardia and ventricular ﬁbrillation, and result in three major symptom complexes — sudden cardiac death, syncope, or minimal symptoms such as dizziness and palpitations. Ventricular tachycardia (Fig. 7.2) is a relatively organized tachyarrhythmia with discrete QRS complexes. It can be either sustained or nonsustained and can be monomorphic or polymorphic — polymorphic ventricular tachycardias tend to be faster and less stable than monomorphic tachycardias. The rate of ventricular tachycardia can be from 100 beats/min to more than 300 beats/min. At slower rates, ventricular tachycardia often does not cause signiﬁcant hemodynamic compromise and may be relatively asymptomatic. The symptoms produced by ventricular tachycardia also depend on the morphology of the tachycardia, the severity of the underlying heart disease, the vascular tone, the geometry of ventricular contraction during the tachycardia, and on whether the patient is upright or supine. At faster rates (usually 220 beats/min or faster), the tachycardia is so rapid that it may be impossible to distinguish the QRS complex from the T waves. This type of ventricular tachycardia is often referred to as ventricular ﬂutter. Ventricular ﬁbrillation (Fig. 7.3) is a completely disorganized tachyarrhythmia without discrete QRS complexes. This arrhythmia causes instant hemodynamic collapse and rapid loss of consciousness because the heart immediately ceases to contract meaningfully. When ventricu-

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Fig. 7.2 Ventricular tachycardia. In unimorphic (or monomorphic) ventricular tachycardia, all QRS complexes are similar in morphology. In polymorphic ventricular tachycardia, the QRS complexes have constantly changing morphologies. In ventricular ﬂutter, the ventricular rate is so rapid that the QRS complexes cannot be readily distinguished from T waves.

lar ﬁbrillation begins, it is associated with a coarse electrical pattern. As the heart becomes less viable (over a period of a few minutes), the amplitude of ﬁbrillation waves seen on the ECG becomes ﬁner and ﬁner. Finally, all electrical activity ceases (ﬂat-line). Recordings from patients who have worn Holter monitors at the time of sudden cardiac death have often displayed the following progression of arrhythmias (Fig. 7.4): An acute increase in ventricular ectopy is followed within a few seconds to minutes by ventricular tachycardia, which in turn degenerates (again in seconds to minutes) to coarse and then ﬁne ventricular ﬁbrillation. Five to seven minutes later, there is no electrical activity. Patients who are successfully resuscitated during such an episode (electrophysiologists have called them, oxymoronically, “sudden death survivors”) are often labeled as having had primary ventricular ﬁbrillation because that is the rhythm commonly seen by the time rescuers arrive. If the rescuers are a little too late, they see the

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Fig. 7.3 Ventricular ﬁbrillation. Ventricular ﬁbrillation is a completely chaotic ventricular rhythm without discernible QRS complexes.

Fig. 7.4 A typical sequence of events in sudden death. This ﬁgure shows tracings from a Holter recording made in a patient who experienced sudden death. At 12:01 PM the patients is in sinus rhythm with PVCs. At 12:03 PM ventricular tachycardia occurs, which degenerates to ventricular ﬁbrillation at 12:05 PM. By 12:08 PM, ﬁne ventricular ﬁbrillation is present. All electrical activity has ceased by 12:10 PM.

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ﬂat-line pattern of the dead heart. This has led to the popular misconception that sudden bradycardia is responsible for a large proportion of sudden deaths. The one-year risk of arrhythmia recurrence for sudden death survivors is between 30% and 50%. Most recurrences are fatal. When syncope occurs in a patient who has a history of previous myocardial infarction or cardiomyopathy (especially if complex ventricular ectopy is present), a spontaneously terminating ventricular tachyarrhythmia must be high on the list of differential diagnoses. Such patients have up to a 50% chance of having inducible ventricular tachycardia during electrophysiologic testing, and those who have inducible arrhythmias subsequently have a high risk of sudden death (nearly as high as in sudden death survivors). It is unlikely that a patient will survive multiple episodes of hemodynamically unstable (i.e., syncope-producing) ventricular arrhythmias. Indeed, patients with underlying heart disease who present with a single syncopal episode actually have a worse prognosis than patients who present with multiple syncopal episodes. (In these latter patients, there is likely to be some other cause for the syncope.) Despite the fact that reentrant ventricular tachyarrhythmias are responsible for hundreds of thousands of sudden deaths each year in the United States, it is not unusual for sustained reentrant ventricular tachycardia to present with relatively minimal symptoms (minimal symptoms being palpitations, dizziness, lightheadedness, and other minor symptoms that are less severe than loss of consciousness). Sustained ventricular tachycardia that produces only minimal symptoms almost invariably presents as a monomorphic wide-complex tachycardia whose rate is less than 200 beats/min. Patients who present with these minimally symptomatic arrhythmias have a lower risk of sudden death than patients who have lost consciousness with their presenting arrhythmias — but their risk is still far higher than normal. Owing to the lack of severe symptoms, a major problem that occurs with these patients is that physicians often mistake their relatively welltolerated ventricular tachycardia for supraventricular tachycardia with aberrancy. At some time in their careers, all physicians memorize a list of clues that helps them to distinguish ventricular tachycardia from supraventricular tachycardia with aberrancy in patients presenting with wide-complex tachycardia. Such a list of clues is presented in Table 7.3. Unfortunately, within 15 minutes of taking the examination for which they memorized those clues, most physicians forget all of them. Instead, they often substitute the following simple rule (because it is easy to remember): “Ventricular tachycardia always causes loss of consciousness”. This tenet is patently false and often leads to mistaking

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Table 7.3 Clues for Distinguishing Ventricular Tachycardia from Supraventricular Tachycardia with Aberrancy.

AV dissociation present QRS duration Precordial concordance If RBBB conﬁguration: lead V1 lead V6

If LBBB conﬁguration: lead V1

Ventricular tachycardia

Supraventricular tachycardia with aberrancy

50% Often > 0.14 sec Often present

Never Often < 0.14 sec Usually not present

Initial R taller (Rsr) Monophasic QRS common Axis commonly < −30º

Second R taller (rsR) Triphasic QRS common Axis usually > −30º

Wide R wave, >0.04 sec

Narrow R wave

concordance, either all QRS complexes are positive, or all are negative. RBBB, right bundle branch block; LBBB, left bundle branch block.

sustained ventricular tachycardia for paroxysmal atrial tachycardia (PAT) with aberrancy. Patients thus misdiagnosed are then sent out of the emergency room without appropriate treatment. Because their reentrant ventricular tachycardia is not recognized, the opportunity to intervene to reduce their long-term risk of sudden death is missed. Intravenous adenosine has come into common usage for termination of supraventricular tachycardias and thus is often administered to patients with wide-QRS-complex tachycardia. When adenosine is administered, useful clues can often be seen that can lead one to a diagnosis of ventricular tachycardia. When supraventricular tachycardia of any type is treated with adenosine, careful observation usually reveals some transient change in the rhythm, even if the supraventricular tachycardia is not terminated. For instance, patients with atrial ﬂutter or atrial tachycardia most commonly will have transient second- or thirddegree AV block following IV adenosine, thus revealing the underlying mechanism of the arrhythmia. In contrast (unless the patient has one of the rare forms of ventricular tachycardia that responds to verapamil and adenosine), when adenosine is administered to a patient with ventricular tachycardia, nothing happens. Thus, when a patient with widecomplex tachycardia has no response at all to adenosine, ventricular tachycardia should immediately become the leading diagnosis. Because the clues listed in Table 7.3 are difﬁcult to remember, the author proposes an alternative simple rule:

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When patients with previous myocardial infarction or cardiomyopathy present with wide-complex tachycardia, it is ALWAYS ventricular tachycardia, regardless of symptoms.

This rule will lead to the correct diagnosis in more than 95% of patients with underlying cardiac disease who present with wide-complex tachycardia. If such patients are referred for a more aggressive evaluation, the few who do have supraventricular arrhythmias will be diagnosed during electrophysiologic testing. The electrophysiologic study in the evaluation of reentrant ventricular tachyarrhythmias

The electrophysiology study has revolutionized our understanding and management of lethal ventricular arrhythmias. Through the electrophysiology study, we have come to learn that most patients with ventricular tachyarrhythmias have reentrant foci as the source of their arrhythmias; that the arrhythmias can be reproduced safely in the laboratory; that some reentrant circuits can be successfully ablated using transcatheter techniques; and that no matter how thorough and aggressive one may be in testing antiarrhythmic drugs, these drugs cannot be fully relied upon to protect against recurrent ventricular arrhythmias. The reasons for performing electrophysiology studies in patients known or suspected to have sustained ventricular tachyarrhythmias are: 1) To diagnose the presence of a reentrant circuit that can cause a ventricular tachyarrhythmia; 2) to test the effect of antiarrhythmic drugs on the inducible arrhythmias; 3) to assess the feasibility of mapping and ablating a reentrant circuit; and 4) to optimize the programming of an antitachycardia device. Inducing ventricular arrhythmias In considering the techniques used for inducing ventricular arrhythmias, we should begin by reviewing the prerequisites for reentry. First, an appropriate anatomic circuit should be present (see Figure 2.6). Second, the electrophysiologic characteristics of the circuit should be such that an appropriately timed premature impulse can block down one pathway (pathway B) and conduct down the other pathway (pathway A) to establish a continuously circulating impulse. Third, the initiating premature impulse must reach the circuit at a critical instant in time (i.e., when pathway B is refractory and pathway A has recovered). The successful induction of ventricular tachycardia in the electrophysiology laboratory depends on the ﬁrst two prerequisites being in place: An anatomic circuit with appropriate electrophysiologic characteristics must be present. The only prerequisite for reentry supplied by

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the electrophysiologist is the critically timed premature impulse. By programmed stimulation, the electrophysiologist attempts to deliver a premature impulse to the reentrant circuit at just the right moment to induce ventricular tachycardia. Delivering a premature impulse to a reentrant circuit at just the right moment is sometimes not easy. As noted in Chapter 4, the distance between the pacing electrode and the reentrant circuit, as well as the refractory characteristics and conduction velocity (i.e., the functional refractory period [FRP]) of the intervening tissue, determine whether it is possible for a paced impulse to reach the reentrant circuit early enough to initiate an arrhythmia. Unfortunately, the precise location of the suspected reentrant circuit is almost always unknown, and the FRP of the tissue between the pacing electrode and the reentrant circuit cannot be measured. Thus, the measures used to optimize conditions to allow premature paced impulses to arrive at the reentrant circuit early enough to initiate reentry are necessarily empiric. As we have seen, pacing at faster rates (i.e., at shorter cycle lengths) decreases the refractory periods and increases the conduction velocity in ventricular myocardium, thus decreasing the FRP. Shorter FRPs will allow premature impulses to arrive at the reentrant circuit earlier and will increase the chances of initiating reentry. Stimulation protocols use two basic techniques to minimize the FRP of the ventricular myocardium: Coupling multiple premature impulses together (typically up to three programmed extrastimuli) and pacing incrementally at rapid rates. In addition, most stimulation protocols call for pacing from more than one catheter location, on the simple premise that one location may be closer to a reentrant circuit than another. Typically, pacing is performed initially from the right ventricular apex, and if no arrhythmias are induced, the electrode catheter is moved to the right ventricular outﬂow tract and pacing is repeated. Some electrophysiologists will also pace from the left ventricle. The experience of most, however, is that left ventricular stimulation is unlikely to induce an arrhythmia if no arrhythmias have been inducible from two right ventricular sites. Finally, the inducibility of a reentrant ventricular arrhythmia can occasionally be improved by infusing isoproterenol. Presumably, in some patients, catecholamines act on potentially reentrant circuits to optimize the electrophysiologic characteristics for reentry. Programmed stimulation protocols vary somewhat from institution to institution. The basic organization of stimulation protocols is to use progressively more aggressive pacing techniques, until either the desired

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arrhythmia is induced or the protocol is ﬁnished (in which case the patient is declared to be non-inducible). A typical stimulation protocol is outlined in Table 7.4. The electrode catheter is initially positioned in the right ventricular apex. Following a drive train of eight incrementally paced beats (S1 beats) at a cycle length of 600 msec, a single programmed extrastimulus (S2) is introduced at a coupling interval of 500 msec (Fig. 7.5A). If no arrhythmia is induced, the pacing sequence is repeated. With each pacing sequence, the coupling interval between the last S1 stimulus and the S2 stimulus is decreased by 10–20 msec, until the S2 no longer captures (i.e., the effective refractory period [ERP] for the S2 is reached). This procedure is then repeated, with S1 drive train cycle lengths of 500 msec, then 400 msec. If no ventricular tachycardia is induced with single extrastimuli at any of the three drive cycle lengths, the S2 stimulus is “parked” at a coupling interval approximately 20 msec longer than its ERP and a second extrastimulus (an S3) is added (Figure 7.5B). At drive cycle lengths of 600, 500, and 400 msec, the S1–S2–S3 coupling intervals are brought in as closely as possible. If double extrastimuli also fail to induce the arrhythmia, a third extra stimulus is added (S4; Figure 7.5C). At drive trains of 600, 500, and 400 msec, the S1–S2–S3–S4 intervals are brought in as tightly as possible. If no ventricular tachycardia is induced with single, double, or triple extrastimuli at any of the three drive cycle lengths, incremental pacing is performed. Incremental trains consisting of 8–12 stimuli are introduced with progressively shorter cycle Table 7.4 A Typical Stimulation Protocol. End points for the electrophysiology study • >10 beats of reproducibly inducible ventricular tachycardia (positive study)* • completing protocol without inducing ventricular tachycardia (negative study) The following pacing sequences are introduced from the right ventricular apex Step 1: single extrastimulus brought in to ventricular refractoriness at 3 drive cycle lengths Step 2: double extrastimuli brought in to ventricular refractoriness at 3 drive cycle lengths Step 3: triple extrastimuli brought in to ventricular refractoriness at 3 drive cycle lengths Step 4: 8–12 incrementally paced beats brought in to ventricular refractoriness If ventricular tachycardia not induced, these steps are repeated from the right ventricular outﬂow tract. If ventricular tachycardia still not induced, isoproterenol is infused and pacing repeated. *Many authorities requires 30 sec of induced ventricular tachycardia to consider a test positive.

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Fig. 7.5 Typical stimulation protocol for inducing ventricular tachycardia. Right ventricular pacing is illustrated. (A) Pacing begins with the introduction of a single extrastimulus (S2) following drive trains of incrementally paced beats (S1). (B) If ventricular tachycardia is not induced, two extrastimuli are used (S3). (C) If ventricular tachycardia is not induced with two extrastimuli, three extrastimuli are used (S4). (D) If ventricular tachycardia is still not induced, incremental bursts are used.

lengths, beginning at a cycle length of 350 msec and decreasing to ventricular refractoriness (Figure 7.5D). If no ventricular tachycardia is induced from the right ventricular apex, the electrode catheter is repositioned to the right ventricular outﬂow tract, and the entire stimulation sequence is repeated. If ventricular tachycardia is not induced, an isoproterenol infusion is begun (to produce sinus tachycardia of 110–140 beats/min), and the entire stimulation sequence is repeated. If no ventricular tachycardia has been induced with any of these measures, the patient is deemed to be “non-inducible”. We touch here on the endearing notion that the electrophysiology study deﬁnes the patient deﬁnitively as being in one of two states — inducible or non-inducible. While this conceptualization is fundamentally ﬂawed (as will be discussed in a later section,) it is still clinically useful in many cases. For instance, the electrophysiology study is often performed for diagnostic purposes. The whole point of doing the study here is to see whether an arrhythmia is inducible or not. If it is, then the patient is presumed to have a high probability of developing spontaneous ventricular tachyarrhythmias; and if it is not, that probability is presumed to be low. Perhaps the best example of such a diagnostic study is the use of electrophysiologic testing for syncope of unknown origin. (The evaluation of syncope will be covered in Chapter 10.) Obviously, in such diagnostic

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tests, one wants the stimulation protocol to have a very high chance of inducing arrhythmias that are clinically relevant, but a very low chance of inducing arrhythmias that are never likely to become clinically manifest. No two electrophysiologists completely agree on the “best” stimulation protocol or on the correct deﬁnition of inducibility. Although ideally one wishes to minimize both false positives and false negatives, in reality, when the electrophysiologist selects a stimulation protocol and a deﬁnition of inducibility, he or she is deciding whether to err on the side of producing more false positives (inducing nonclinical arrhythmias, which can lead to inappropriately aggressive therapy) or more false negatives (failing to induce truly clinical arrhythmias, leading to undertreatment). The aggressive stimulation protocol outlined in Table 7.4 errs on the side of producing more false positives. Studies in ostensibly normal patients suggest that in a substantial minority (20–30%), more than 10 beats of polymorphic ventricular tachycardia can be induced when triple extrastimuli are used, but that virtually none have inducible arrhythmias when only double extrastimuli are used. Thus, stimulation protocols using triple extrastimuli are likely to produce some false positive studies. On the other hand, many patients who have had documented sustained ventricular tachyarrhythmias require triple extrastimuli to induce the clinical arrhythmias. Thus, stimulation protocols using less than three extrastimuli will tend to eliminate false positives but will miss some of the true positives. Any deﬁnition chosen for inducibility necessarily takes into account the morphology and the duration of the induced arrhythmia. The morphology of the induced arrhythmia is an issue because the studies in “normals” mentioned earlier suggest that when a false positive ventricular tachycardia is induced, the arrhythmia is almost always polymorphic. Thus, an induced arrhythmia that is polymorphic tends to be nonspeciﬁc. Some institutions accordingly attempt to limit their false positive studies by stipulating that for a study to be considered positive, inducible ventricular tachycardia must be monomorphic. However, although induced polymorphic tachycardia is nonspeciﬁc, patients do, in fact, develop spontaneous polymorphic ventricular tachycardias. Insisting on a monomorphic arrhythmia will thus cause one to ignore some true positive studies. Regarding the duration of the induced tachycardia, most electrophysiologists recognize that in a substantial minority of patients presenting with sustained arrhythmias, only a nonsustained tachycardia will be inducible in the electrophysiology laboratory. Therefore, most laborato-

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ries will accept nonsustained tachycardia (if it is of sufﬁcient duration) as a positive study. The determination of how many beats in duration that nonsustained tachycardia should be is completely empiric. In many laboratories, an inducible arrhythmia is deﬁned by the ability to reproducibly induce at least ten beats of ventricular tachycardia (Fig. 7.6). The number ten is chosen arbitrarily. Some electrophysiologists consider anywhere from three to 15 beats of induced tachycardia to represent a positive study. Others require at least 30 seconds of ventricular tachycardia before an arrhythmia is considered inducible. One must be mindful of Baye’s theorem when deciding on an appropriate stimulation protocol and deﬁnition of inducibility. Baye’s theorem states that the speciﬁcity of any test is determined largely by the true incidence of the condition for which the test is being performed in the population being tested. In electrophysiology studies in patients who present with spontaneous sustained ventricular tachyarrhythmias, it is appropriate to use a more aggressive stimulation protocol and a more liberal deﬁnition of inducibility. In such patients, positive tests are statistically less likely to be falsely positive than in the general population, and are more likely to be truly positive. If programmed stimulation is to be used in patients who are in lower risk groups (such as patients with syncope of unknown origin), it might be reasonable to use a less aggressive pacing protocol and a stricter deﬁnition of inducibility, because the odds of a positive study being falsely positive are higher in such patients.

Fig. 7.6 Types of inducible ventricular tachycardia. When inducing ventricular tachycardia in the electrophysiology laboratory, the goal is to induce sustained monomorphic ventricular tachycardia (shown in the top panel). This response is considered to be speciﬁc. The middle and bottom panels display two induced arrhythmias (nonsustained monomorphic ventricular tachycardia and polymorphic ventricular tachycardia) whose interpretation is controversial.

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Electrophysiologists have perhaps done too much hand-wringing because they cannot agree on standardized pacing protocols and deﬁnitions of inducibility. They worry that the many differences between centers render the electrophysiologic literature impossible to interpret. The author’s opinion is that, on the contrary, the different approaches being used are not particularly harmful and may, in fact, be beneﬁcial. An appraisal of the literature suggests that results with electrophysiologic testing in patients who present with sustained ventricular arrhythmias are actually quite similar among different centers. This suggests that in high-yield patient populations the variations in methodology have not been signiﬁcant. Further, as noted previously, different approaches will probably be of beneﬁt when the electrophysiology study is applied to different patient populations. It may be harmful to be locked into a standardized protocol that may err too much on the side of either false positive or false negative studies when studying new populations. Table 7.5 summarizes the factors that must be considered when estimating the speciﬁcity of the electrophysiology study. Terminating ventricular arrhythmias Termination of induced ventricular tachyarrhythmias is accomplished by one of two methods: Programmed stimulation (possible only with ventricular tachycardia, not with ventricular ﬁbrillation) or direct current (DC) cardioversion/deﬁbrillation. Terminating a reentrant arrhythmia with programmed stimulation requires that a premature impulse encounters the reentrant circuit at a critical time. In this way, initiating and terminating reentry are similar; and the considerations for inducing arrhythmias discussed earlier (i.e., the distance between the electrode catheter and the reentrant circuit on one hand, and the FRP of the intervening tissue on the other)

Table 7.5 Estimating the Speciﬁcity of a Positive Electrophysiology Study. Factors increasing speciﬁcity of a positive study Induced arrhythmia is monomorphic ventricular tachycardia Induced ventricular tachycardia is sustained Tachycardia is induced with single or double extrastimuli Patient studied is in high-risk group Factors decreasing speciﬁcity of a positive study Induced arrhythmia is polymorphic ventricular tachycardia or ventricular ﬁbrillation Induced arrhythmia is nonsustained Arrhythmia is induced with triple extrastimuli or incremental pacing Patient studied is not in high-risk group

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also pertain to termination of the tachycardia. Thus, techniques for pace-termination of ventricular tachycardia are similar to techniques for pace-induction. Several methods for pace-termination of ventricular tachycardia have been proposed, but they essentially boil down to the incremental and extrastimulus techniques that we have seen before (Fig. 7.7). The incremental method is used most commonly. Generally, incremental pacing to terminate ventricular tachycardia begins with 8–12 beats at a cycle length 10–20 msec faster than the cycle length of the tachycardia. If this is unsuccessful, pacing is repeated at faster rates. When the extrastimulus technique is used to terminate ventricular tachycardia, the extrastimuli are generally coupled to the intrinsic tachycardia beats rather than to a train of incrementally paced beats. Whichever pacing method is used to terminate ventricular tachycardia, there is a real risk of accelerating the tachycardia or causing it to degenerate to ventricular ﬁbrillation (Fig. 7.8). This poor result tends to occur more frequently with more aggressive pace-termination measures (such as rapid incremental pacing or triple extrastimuli), but these

Fig. 7.7 Pace-termination of ventricular tachycardia. The top panel shows termination of ventricular tachycardia using a six-beat burst of incremental stimuli. The bottom panel shows termination of ventricular tachycardia using three programmed extrastimuli.

Fig. 7.8 Degeneration of ventricular tachycardia with pacing. This ﬁgure shows one of the inherent hazards in attempting to pace-terminate ventricular tachycardia. In this example, a six-beat burst of incremental stimuli degenerates the ventricular tachycardia into ventricular ﬁbrillation.

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more aggressive pacing measures are also the most efﬁcacious at terminating the tachycardia. If degeneration of the rhythm results from efforts at pace-termination, the patient usually needs to be rescued with a DC shock. Successful pace-termination of ventricular tachycardia is easier to accomplish with arrhythmias that are relatively slow and monomorphic. The faster and less organized the arrhythmia, the harder it is to pace-terminate. The choice of the timing and method of terminating the induced arrhythmia depends on several factors, including the rate and morphology of the induced arrhythmia, the duration of the arrhythmia, the blood pressure, and the patient’s symptoms and level of consciousness. In most laboratories, if the patient is tolerating the induced ventricular tachycardia, no attempt will be made to terminate the arrhythmia for 30 seconds (both, in order to assess the patient’s tolerance of the arrhythmia, and to see if the arrhythmia will terminate spontaneously). If the patient is awake but uncomfortable (experiencing lightheadedness, severe palpitations, or angina) or severely hypotensive, the electrophysiologist immediately attempts to pace-terminate the arrhythmia. If at any time the patient becomes unconscious, a DC shock is delivered. In most laboratories, once attempts to terminate the arrhythmia are begun, patients remain in ventricular tachycardia for an average of less than 10–15 seconds. Deaths from inducing ventricular arrhythmias in the electrophysiology laboratory are extremely rare (<0.01%,) and even the need for full cardiopulmonary resuscitation is very uncommon (<0.10%). Testing the effect of drugs on the reentrant circuit From the early 1980s until the mid 1990s, serial drug testing was the major reason for studying patients with reentrant ventricular tachyarrhythmias. This practice has largely fallen away for two reasons. First, large studies showed that pharmacologic therapy based on serial drug testing was not nearly as effective as had previously been thought. Second, results obtained with the implantable cardioverter– deﬁbrillator (ICD) were far better than with serial drug testing — or with any other treatment. Today, serial drug testing is done only rarely, and is generally limited to patients who refuse therapy with the ICD, or for whom the intention is to reduce the frequency of recurrent arrhythmias in the presence of an ICD. The principle behind drug testing for ventricular tachyarrhythmias is simple. As discussed in Chapter 3, antiarrhythmic drugs work by changing the shape of the cardiac action potential, thus altering the conduc-

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tion velocity or refractoriness of cardiac tissue. By so doing, these drugs are capable of altering the electrophysiologic properties of a reentrant circuit to make a reentrant arrhythmia less (or more) likely to occur. If a ventricular arrhythmia that was inducible during baseline (drug-free) testing is no longer inducible after administering a drug, then that drug has probably had a favorable effect on the reentrant circuit (Fig. 7.9). For years, it was thought that treatment with a drug that rendered a previously inducible arrhythmia non-inducible would protect against recurrent arrhythmias. As it turns out, a drug deﬁned as being “successful” during serial drug testing probably delays the onset of an arrhythmia, but may not substantially reduce the long-term risk. In the era of widespread serial drug testing, most centers averaged approximately three drug trials per patient and found successful drugs in 30–40% of patients tested. In some centers, no more than one or two drug studies were performed before moving directly to nonpharmacologic therapies. In other centers, exhaustive drug trials were carried out, including studies with multiple drug combinations. Despite differences in stimulation protocols, deﬁnitions of inducibility, and the number of drug studies performed, the long-term outcomes for patients who responded to drug testing and for patients who did not respond to drug testing were similar from center to center. Drug responders appeared to have a lower rate of recurrent arrhythmias than nonresponders (approximately 5–10% per year versus 30–50% per year). Unfortunately, since most recurrences were fatal, the proportion of surviving patients at the end of ﬁve years was similar in both groups.

Fig. 7.9 Successful serial drug testing for ventricular tachycardia. At baseline (top panel) and after administration of procainamide (middle panel), sustained ventricular tachycardia is inducible. After administration of quinidine (bottom panel), however, no ventricular tachycardia is inducible. Quinidine would appear to have a favorable effect on the reentrant circuit in this patient.

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The meaning of “inducibility” and “non-inducibility” The fact that serial drug testing is no longer commonly performed has signiﬁcantly limited the use of the electrophysiology study in patients with ventricular arrhythmias. One remaining use, however, is diagnostic — that is, in the assessment of patients who are thought, but not known beyond doubt, to have ventricular arrhythmias. (The best example is in the case of patients with syncope of unknown origin, discussed in Chapter 10.) Especially in such cases, it is important to understand what “inducibility” and “non-inducibility” really means. Earlier, we suggested that many electrophysiologists believe that the electrophysiology study sorts patients into one of two states: Inducible or non-inducible. If they are inducible, they have a potentially lethal reentrant circuit. If they are non-inducible, then either they do not have such a circuit, or something that the doctor did (like administer an antiarrhythmic drug) has effectively rendered their reentrant circuit nonfunctional. In other words, the “inducibility state” of the patient is thought of as a binary and deterministic feature, which is deﬁned by the electrophysiology study. Several years ago, the author conducted a study to test this proposition. In this study, patients with inducible ventricular tachycardia which was made non-inducible during serial drug testing were immediately subjected to ﬁve additional, complete stimulation protocols over the next 24 hours, while being given the drug that had suppressed their inducible tachycardia. It turned out that the probability of inducing ventricular tachycardia during any one of the ﬁve subsequent drug trials remained constant — roughly 15–20%. In other words, the odds of failing trial number two (after having passed only one previous trial) was the same as the odds of failing trial number six (after having passed ﬁve previous trials). Such results strongly suggest that the inducibility of reentrant arrhythmias does not deﬁne a clear-cut binary state — that patients are not either inducible or non-inducible; but this suggests instead that inducibility is best regarded as a probability function, not as a deterministic state. This ﬁnding makes perfect sense when one considers that virtually all complex, multifactorial, physiologic events follow a probabilistic “doseresponse” curve, in which a given “dose” of a stimulus yields a measurable probability that an event will occur. Figure 7.10 postulates such a probability curve for the induction of ventricular tachycardia. In this model, a successful drug trial merely implies that the probability curve has been shifted to the right. Another way of looking at the probabilistic nature of inducibility is illustrated by what the author calls the “dunk tank model” of reentrant

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Fig. 7.10 The probabilistic nature of the inducibility of ventricular tachycardia. It is postulated that probability of inducing ventricular tachycardia (VT) follows a typical S-shaped curve, similar to the probability functions that describe most physiologic systems. In this model, a drug that prevents inducibility in the electrophysiology laboratory has merely shifted the curve to the right, so that with a ﬁxed amount of stimulation the probability of inducing the arrhythmia is diminished.

ventricular tachycardia (Fig. 7.11). In this model, the patient with ventricular tachycardia can be visualized as sitting on a typical dunk tank platform (except, of course, this dunk tank is ﬁlled not with water but with boiling oil). The patient’s reentrant circuit is analogous to the target-platform mechanism, and the triggering electrical impulse (a PVC or paced beat) is analogous to the softballs that one throws at the target. In the baseline state (Figure 7.11A), the target is close enough for the thrower to have an excellent chance of hitting it with one allotment of softballs (or with one stimulation protocol). This patient would be called inducible. An “effective” antiarrhythmic drug can be visua lized as moving the target farther away (Figure 7.11B), so that the probability of striking the target with one allotment of softballs has been substantially reduced (say, to 15%). This patient would be labeled noninducible. If one, however, were to keep buying more softballs to throw, the cumulative probability of hitting the target would gradually and inexorably increase. This model ﬁts not only our experimental data but also the clinical results seen with serial drug testing. The probability that a fatal ventricular arrhythmia will occur over any given time interval is reduced after “successful” serial drug testing — but the overall, cumulative

Fig. 7.11 The dunk tank model of ventricular tachycardia. This ﬁgure presents a different way of illustrating the probabilistic nature of ventricular tachycardia. (A) The patient with ventricular tachycardia is visualized as sitting on a dunk tank platform. The target-platform mechanism represents the reentrant circuit, and the softballs that one throws at the target represent ventricular ectopy (or the premature beats introduced by the electrophysiologist). In (A), the target is close enough to the thrower that the probability of “dunking” the patient with a single allotment of softballs is relatively high. (B) The proposed effect of a “successful” antiarrhythmic drug. The target is far enough away from the thrower that it is unlikely that the target will be struck with a single allotment of softballs. However, if one is persistent in throwing at the target, sooner or later the patient will wind up in the drink.

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probability of having an arrhythmia (as more and more time intervals accumulate) remains high. Viewing the inducibility status of a patient from this point of view does not render the electrophysiology study useless. On the contrary, it offers a more realistic perspective (than does the binary, deterministic model) from which to interpret the results of an electrophysiology study, whether that study is a serial drug test, or a diagnostic procedure. As with any test performed in medicine, it is important for the doctor to understand the inherent limitations and beneﬁts of the electrophysiology study, so as to provide more appropriate clinical recommendations. The electrophysiology study in the treatment of reentrant ventricular tachyarrhythmias

While in the recent past, performing electrophysiologic testing was considered standard care in the management of sustained ventricular arrhythmias, this is not the case today. Nonetheless, the electrophysiology study can still be quite useful in helping to treat ventricular arrhythmias in at least two ways: First, the electrophysiology study plays an essential role in the transcatheter ablation of ventricular arrhythmias. This technique will be discussed in Chapter 8. Second, electrophysiologic testing can be useful in tailoring the way that ICDs are programmed to handle recurrent arrhythmias. Pre-operative electrophysiologic testing for ICDs Appropriately programming ICDs often requires several complex decisions. One such decision is whether and how to use antitachycardia pacing (ATP) to terminate recurrent ventricular tachycardia. In programming ATP, the physician sets a rate zone in which ATP is to be attempted. For instance, one might choose to attempt ATP for arrhythmias whose rate is between 150 and 190 beats/min. If a ventricular tachycardia of more than 190 beats/min would occur, ATP would not be used — a DC shock would be administered instead. A shock would also be given if a pre-selected number of ATP attempts failed to stop a ventricular tachycardia, or if the arrhythmia were to accelerate with an ATP attempt. Programming ATP inappropriately can lead to serious problems. Because ATP is a potentially “kinder, gentler” therapy, the physician may be tempted to try it even for rapid, hemodynamically unstable tachycardias that would otherwise be treated immediately with high-energy shocks. Because rapid tachycardias are (most electrophysiologists agree) more difﬁcult to terminate with ATP than slower

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tachycardias, prolonged attempts at ATP could conceivably allow prolonged hemodynamic compromise before “deﬁnitive” therapy is ﬁnally administered. Conversely, the availability of ATP may tempt physicians to use implantable devices to treat slow, relatively well-tolerated tachycardias that might be better treated by other means. In such cases, the ICD may be programmed to deliver therapy at slower heart rates that are often reached when the patient develops sinus tachycardia or atrial ﬁbrillation, thus potentially triggering inappropriate ATP attempts. Not only will such inappropriate ATP sequences fail to stop the supraventricular tachycardia, but they might also induce the very ventricular tachycardias that they are supposed to terminate. In any case, once an ICD begins delivering therapy, it does not stop until the heart rate falls below the programmed rate cutoff. Thus, unless the supraventricular arrhythmia terminates spontaneously, the device gradually, inexorably, and inappropriately escalates therapy until a series of high-energy shocks are delivered. It is for the purpose of avoiding such problems that some electrophysiologists perform electrophysiologic testing prior to ICD implantation. The purpose of such testing is to characterize the nature of the patient’s sustained ventricular tachycardia — its rate, how well it is tolerated, and what kinds of pacing sequences seem to reliably terminate it. Generally in these tests, ventricular tachycardia is induced and terminated several times in order to characterize the arrhythmia and the response to ATP as fully as possible. Some electrophysiologists feel that pre-ICD testing is extremely useful, and they do it routinely. Other electrophysiologists point out that the characteristics of a patient’s induced ventricular tachycardia is often quite different from their spontaneous tachycardia, and that the odds of successfully pace-terminating a patient’s induced arrhythmia frequently vary from day to day — and thus that the usefulness of pre-op testing is questionable. Further, this species of electrophysiologist feels that one achieves adequate (and even equivalent) success rates simply by programming ATP empirically. The author, having done scores of preoperative electrophysiology studies and observing the results, now tends to agree with the latter electrophysiologists. That being said, many electrophysiologists swear by pre-operative testing, which therefore remains a common and legitimate indication for electrophysiologic testing. Automatic ventricular arrhythmias

Abnormal automaticity accounts for a minority of lethal ventricular tachyarrhythmias. In distinction to reentrant ventricular arrhythmias,

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which are almost always associated with chronic, underlying disease of the myocardium, automatic ventricular arrhythmias tend to be associated with acute, reversible medical conditions, such as acute myocardial ischemia, hypoxemia, acid–base disturbances, electrolyte abnormalities (especially hypokalemia and hypomagnesemia), and high adrenergic tone. Thus, automatic ventricular arrhythmias tend to be seen in two general clinical settings: In patients who are acutely ill (e.g., in the intensive care setting) and in patients who are having acute myocardial ischemia or infarction. It can be argued that patients who are desperately ill in the intensive care unit are not candidates for truly “sudden” death, and, indeed, these patients are not included in most of the statistics on sudden death. On the other hand, lethal arrhythmias secondary to acute myocardial ischemia or infarction can and do occur “suddenly”. The automatic ventricular arrhythmias that occur during the ﬁrst 24–48 hours after an acute myocardial infarction are thought to account for about 20% of the sudden cardiac deaths in the United States. The major success of the coronary care unit has been in preventing these early arrhythmic deaths (although, unfortunately, many of these arrhythmias occur within the ﬁrst hour after an acute infarction — often before the patient has access to modern facilities). The automatic arrhythmias seen during the ﬁrst day or two after an acute myocardial infarction are probably related to the residual ischemia seen acutely in the zone of infarction. Once the infarction heals, the substrate for these early arrhythmias disappears. Therefore, the automatic ventricular arrhythmias that occur early during an acute myocardial infarction are thought to have little long-term prognostic signiﬁcance (provided, of course, that the patient survives them). Because automatic arrhythmias generally occur secondarily to metabolic abnormalities, treatment should be aimed at identifying and reversing the underlying cause whenever possible. In many instances, intravenous antiarrhythmic drugs (particularly lidocaine, phenytoin, and amiodarone) can be helpful in temporarily suppressing automaticity while the primary problem is being addressed. Automatic ventricular arrhythmias are not inducible in the electrophysiology laboratory and the electrophysiology study is not useful in their evaluation or treatment. Triggered activity

As noted in Chapter 2, triggered activity is a mechanism for ventricular arrhythmias that has features of both automaticity and reentry. In recent years, the clinical features of arrhythmias mediated by triggered activity

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have been better characterized. Although triggered activity is a relatively uncommon cause of ventricular arrhythmias, the clinician must be alert to such arrhythmias for two reasons. First, these arrhythmias, like any ventricular tachyarrhythmia, are life-threatening. Second, the successful treatment of arrhythmias mediated by triggered activity can be uniquely different from treatment used for other forms of ventricular arrhythmias. Two fairly distinct clinical syndromes have been identiﬁed involving triggered activity: Pause-dependent arrhythmias and catecholdependent arrhythmias. In each syndrome, patients develop the polymorphic ventricular tachycardias that have been called torsade de pointes. Although the arrhythmias tend to occur in relatively short bursts and are usually accompanied by lightheadedness or syncope, the arrhythmias can persist long enough to cause sudden death. Pause-dependent triggered activity

Pause-dependent triggered activity is caused by afterdepolarizations that occur during phase 3 of the cardiac action potential; hence they are called early afterdepolarizations (EADs; Fig. 7.12A). If the afterdepolarization reaches the threshold potential of the cardiac cell, another action potential can be generated. Pause-dependent triggered activity is almost always related to conditions that prolong the duration of the cardiac action potential, such as electrolyte abnormalities (hypokalemia and hypomagnesemia), and the use of class Ia or class III antiarrhythmic agents. Individuals who develop triggered arrhythmias when their QT intervals are prolonged most likely have an inborn sub-clinical abnormality of the cardiac cell membrane, which becomes manifest only when their action potential durations are increased. The ventricular arrhythmias themselves (referred to as torsade de pointes) are typically polymorphic and tend to occur in short bursts. The ECG while in sinus rhythm usually shows prolongation of the QT interval and distortion of the T wave; often, a distinct U wave occurs. During studies using the monophasic action potential, Warren Jackman at the University of Oklahoma has convincingly shown that the U waves are, in fact, the ECG manifestation of the EADs themselves. When a burst of ventricular tachycardia occurs, the ﬁrst beat of tachycardia is invariably superimposed on the U wave (or the distorted T wave), suggesting that the EAD (represented by that U wave) has reached the transmembrane potential for generating an action potential (Fig. 7.13). The TU wave abnormalities in this condition are usually dynamic. They tend to wax and wane, depending largely on the previous cycle length; the longer the previous cycle length, the more exaggerated the

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Fig. 7.12 Afterdepolarizations. (A) An early afterdepolarization (EAD), the type of afterdepolarization associated with pause-dependent triggered activity. EADs occur during phase 3 of the action potential. (B) A delayed afterdepolarization (DAD), the type associated with catechol-dependent triggered activity. DADs occur after the end of phase 3.

TU wave aberration of the following complex — hence, the condition is “pause dependent.” Once a burst of ventricular tachycardia has been initiated, it tends to repeat in a pattern of “ventricular tachycardia bigeminy” — the burst of ventricular tachycardia causes a compensatory pause, and that pause causes the following sinus beat to develop marked U wave abnormalities (i.e., a pronounced EAD occurs). Thus, another burst of tachycardia is generated after that ﬁrst sinus beat. Pausedependent triggered activity should be strongly suspected when this

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Fig. 7.13 The relationship between early afterdepolarizations (EADs), TU wave abnormalities, and premature ventricular complexes. (A) The temporal association between EADs and the TU abnormalities as seen on the surface ECG. The TU wave is most likely the surface manifestation of the EADs themselves. (B) If an EAD is of sufﬁcient magnitude to reach threshold potential, a premature complex results. Note that the timing of the premature complex is such that it occurs precisely on the TU wave of the previous beat.

ECG pattern occurs either in the setting of QT interval prolongation or in the setting of conditions that predispose to QT interval prolongation, even if overt QT prolongation is not present (Fig. 7.14). The treatment of pause-dependent triggered activity is aimed at reducing the duration of the action potential. Drugs that prolong the QT interval should be discontinued and avoided — speciﬁcally,

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Fig. 7.14 Ventricular arrhythmias caused by pause-dependent triggered activity (torsade de pointes). Features of pause-dependent ventricular arrhythmias are shown in a patient with QT prolongation from quinidine. In the top panel, “late” premature ventricular complexes (coincident with the onset of the U wave) arise immediately after a relatively long interval (i.e., a “pause”) between QRS complexes. In patients prone to develop these arrhythmias, the pause itself induces afterdepolarizations (see text), thus triggering ectopic complexes. The bigeminal pattern seen here is typical, because each ectopic complex tends to produce a compensatory pause that, in turn, produces another ectopic complex. In the middle panel, the ectopy has become more sustained. Compensatory pauses still follow each burst of ventricular tachycardia, so that the patient now displays “ventricular tachycardia bigeminy”. In the bottom panel, the arrhythmia has become even more prolonged and now displays a more typical “torsade de pointes” morphology. The key to recognizing torsade de pointes is to recognize the pause-dependent nature of the arrhythmia; the key to treating these arrhythmias is to eliminate the pauses. Thus, overdrive pacing reliably suppresses these arrhythmias.

antiarrhythmic drugs that prolong action potential duration should not be used (drugs that cause this type of triggered activity are listed in Table 3.2). Electrolyte abnormalities should be rapidly corrected. Intravenous magnesium sulfate often ameliorates these arrhythmias, even when the serum magnesium level is not depressed. The mainstay of emergent

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treatment of these arrhythmias, however, is to eliminate pauses; that is, to increase the heart rate. This is usually accomplished either by atrial or ventricular pacing, or by beginning an isoproterenol infusion. Because the conditions that lead to pause-dependent triggered activity are generally reversible, long-term therapy is aimed at avoiding conditions that cause prolongation of the QT interval. Catechol-dependent triggered activity

Catechol-dependent triggered activity is caused by afterdepolarizations that occur during phase 4 of the cardiac action potential (Figure 7.12B). Thus, these afterdepolarizations are called delayed afterdepolarizations (DADs). DADs occur in the setting of digitalis toxicity, in cardiac ischemia, and in some patients who have congenital QT interval prolongation. These congenital syndromes are the Romano-Ward syndrome and the Jervell-Lange-Nielson syndrome (in which QT prolongation is accompanied by neural deafness). Patients with catecholdependent triggered activity have been postulated to have an imbalance in sympathetic innervation of the heart, with predominant input from the left stellate ganglion, stimulation of which can reproduce DADs. Catechol-dependent triggered activity generally is not dependent on pauses (although pause-dependent features are seen in some patients). Instead, they are brought out in conditions of high sympathetic tone. Thus, patients experience ventricular tachycardia (manifested by syncope or cardiac arrest) during times of exercise or of emotional stress. Often, the QT interval is normal at rest. During stress testing, QT prolongation occurs, and often ventricular tachycardia is seen. Left stellate sympathectomy has eliminated arrhythmias in some patients. Treatment of catechol-dependent triggered activity usually consists of βblockers, and, because DADs are thought to be mediated by calciumdependent channels, of calcium channel blockers. In addition, more and more clinicians are using ICDs in these patients. Miscellaneous types of ventricular arrhythmias

Clinical syndromes involving unusual ventricular arrhythmias have been described in which the arrhythmias do not ﬁt clearly into any of the categories described so far. In many cases, these arrhythmias occur in the setting of a structurally normal heart; and in most cases, their mechanisms are not well understood. The literature is confusing regarding their classiﬁcation and nomenclature, which is merely a reﬂection of our incomplete understanding of these arrhythmias. The following is a brief description of these syndromes.

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Idiopathic left ventricular tachycardia

This arrhythmia tends to occur in younger patients without structural heart disease. The arrhythmia has a right bundle branch block morphology with a left, superior axis. It is inducible with programmed stimulation, and each QRS complex is preceded by a distinct His spike. The arrhythmic focus maps to the inferior aspect of the septum, and in several patients it has been successfully ablated. It tends to respond to therapy with β blockers and calcium channel blockers. Both reentry and triggered activity have been advanced as the mechanism of this arrhythmia. Outﬂow tract ventricular tachycardia

This arrhythmia, which has also been termed repetitive monomorphic ventricular tachycardia, originates in the right ventricular outﬂow tract. It manifests as a nonsustained left bundle branch block tachycardia with an inferior axis and is often provoked by exercise. Although the arrhythmia is often not inducible with programmed extrastimuli, pacing the heart at a rapid rate or instituting an isoproterenol infusion (i.e., simulating the heart rate response with exercise) can often induce the arrhythmia. It is usually seen in younger patients without structural heart disease. The arrhythmia tends to be responsive to therapy with β blockers and calcium channel blockers, but the treatment of choice is usually transcatheter ablation, which has a high success rate in completely eliminating the arrhythmia. Whether this arrhythmia represents automaticity or triggered activity is unknown. Right ventricular dysplasia

Right ventricular dysplasia is a rare condition, usually seen in younger patients, in which a variable amount of right ventricular myocardium is replaced by fatty and ﬁbrous tissue. This condition appears to be genetic in origin; recently a genetic mutation has been identiﬁed that accounts for up to 30% of cases. The ventricular tachycardia seen in right ventricular dysplasia usually has a left bundle branch morphology, and is almost invariably inducible with programmed stimulation. The treatment of this arrhythmia is similar to treatment for the reentrant ventricular tachycardias that are seen in the setting of coronary artery disease. Surgery to cause electrical isolation of the dysplastic areas of the right ventricle has been tried, and although it has been successful in controlling the arrhythmia, right ventricular failure commonly follows. Transcatheter ablation of arrhythmogenic foci has been used with some success.

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Bundle branch reentry

Bundle branch reentry is a distinct form of ventricular tachycardia seen rarely in patients with idiopathic cardiomyopathy who also have intraventricular conduction disturbances. Most of these patients present with rapid monomorphic ventricular tachycardia that has a left bundle branch block morphology. The reentrant circuit uses the right bundle branch in the downward direction and the left bundle branch in the upward direction. Its signiﬁcance lies in the fact that it can be cured with the transcatheter ablation of the right bundle branch. Brugada syndrome and sudden unexpected nocturnal death syndrome (SUNDS)

Brugada syndrome was ﬁrst recognized as a clinical complex consisting of ventricular tachyarrhythmias, often presenting as sudden death, cardiac arrest, or syncope, in patients who have unusual baseline ECGs displaying nonischemic ST segment elevation in leads V1–V3 and pseudo-RBBB. These patients are now thought to have genetic abnormalities involving the cardiac sodium channel (the channel that is mostly responsible for depolarization — phase 0 — of the cardiac action potential). Brugada syndrome affects males far more often than females, and the arrhythmias seen with this syndrome frequently occur during sleep. This condition is related to (and may be the same as) the sudden unexpected nocturnal death syndrome (SUNDS) that has been described in apparently health Asian males. There are several variants of the Brugada syndrome, probably reﬂecting various mutations in the cardiac sodium channel gene. In some patients, baseline ST changes are transient, in which case the characteristic ST changes can often be brought out by administering Class I antiarrhythmic drugs (the drugs that operate on the sodium channel) or by pacing or vagal maneuvers. The arrhythmias associated with this syndrome are often inducible with programmed pacing, so a diagnostic electrophysiology study may be useful if Brugada syndrome is suspected. A history of prior cardiac arrest, syncope, or a family history of sudden death, all greatly increase the risk of sudden death in a patient with Brugada syndrome. The only treatment demonstrated to reduce the risk of sudden death in patients with Brugada syndrome is the implantable cardioverter–deﬁbrillator (ICD). Beta blockers and amiodarone have not been shown to protect these patients. The generally accepted approach to treatment is to use clinical parameters to assess the patient’s risk of sudden death and, if the risk is deemed to be relatively high, to insert an ICD.

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Ventricular tachyarrhythmias associated with mitral valve prolapse

Ventricular tachyarrhythmia associated with mitral valve prolapse is mentioned only to point out its minimal signiﬁcance. Although there are many case reports in the medical literature that attribute sudden death to mitral valve prolapse, there is no epidemiologic study that has shown that patients with prolapse are any more susceptible to ventricular tachyarrhythmias than the general population. The purported association between sudden death and prolapse is probably related to the fact that between 5% and 10% of the general population have mitral valve prolapse, so that 5% to 10% of patients with unexplained sudden death are found to have prolapse on autopsy. A perspective on the treatment of ventricular arrhythmias

The optimal treatment of ventricular arrhythmias has changed radically since the ﬁrst edition of this book was published over 15 years ago and has evolved signiﬁcantly even since the last edition appeared only seven years ago. Now, in the ﬁrst decade of the 21st century, thanks to advances in technology and the new knowledge gained from large randomized clinical trials (RCTs), thousands of patients are being offered therapies they could not have received in earlier decades, and they are being kept alive as a result. The progress has been remarkable. At least, that’s one way of looking at it. This would certainly be the view of most electrophysiologists and other cardiologists, professional organizations such as the American College of Cardiology and the Heart Rhythm Society, and federal agencies like the FDA and CMS. Indeed, for any health professional who hopes to make a way for him- or herself within the health care system, especially in an academic environment, seeing our progress in the treatment of ventricular arrhythmias as a model for evidence-based medicine at its ﬁnest is certainly the most advisable approach. The author has a somewhat different perspective on the matter, however, and believes that the approach we have taken in advancing the therapy of ventricular arrhythmias (and thus, our approach to the sudden death problem) actually has not been a particularly enlightened one. In fact, there is a much simpler and more straightforward way of advancing the treatment of ventricular arrhythmias that, if we chose to use it, could be implemented immediately, and over time could save many more lives than we are saving today. Accordingly, the purpose of the following discussion is to suggest a different way of approaching the treatment of ventricular arrhythmias. It is hoped that this new perspective, by throwing into sharp relief the

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reasoning behind and the limitations of our current approach, can help us to understand more readily the continually evolving and often convoluted treatment recommendations being handed down to us; and further, that it can help us distinguish more readily between true scientiﬁc imperatives and dogma. This latter capability will become increasingly important as our society comes to terms with the need to ration health care. Our alternative approach begins with four general truths about treating ventricular arrhythmias. Four general truths about treating ventricular arrhythmias

1) Suppression of ventricular ectopy with antiarrhythmic drugs does not reduce risk As we have noted, in the setting of underlying cardiac disease, complex ventricular ectopy is one of the risk factors for sudden death. For years, it was assumed that antiarrhythmic drugs aimed at suppressing such ectopy would reduce the risk. The medical community was ﬁnally disabused of this benign view of ectopy suppression in 1989, with the results of the Cardiac Arrhythmia Suppression Trial (CAST; Echt DS et al., N Engl J Med 1991; 324:781). CAST was designed to study whether suppressing ventricular ectopy in patients with recent myocardial infarctions reduced the risk of death. What it showed instead was that the successful suppression of ectopy with two of the three drugs studied (encainide and ﬂecainide) actually doubled or tripled the risk of death or cardiac arrest, while successful suppression of ectopy with the third drug (moricizine) provided no survival beneﬁt. There were plenty of other reasons at the time to suspect that using antiarrhythmic drugs to suppress ectopy was risky, but CAST drove home the point — suppression of ambient ventricular ectopy with antiarrhythmic drugs does not lead to a reduction in mortality and in fact may increase mortality. In contrast, the other major method for choosing antiarrhythmic drug therapy — serial drug testing in the electrophysiology laboratory — assessed the effect of antiarrhythmic drugs on the reentrant circuit itself and not merely on ambient ectopy. Drugs selected for chronic administration in this manner rarely produced the sort of proarrhythmia seen in CAST, since most proarrhythmic effects could be identiﬁed in the laboratory, before committing the patient to chronic therapy. Indeed, because such proarrhythmic effects were so frequently identiﬁed during serial drug testing, many electrophysiologists who did this kind of testing were not at all surprised by the results of CAST.

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2) Empiric treatment with amiodarone does not sufﬁciently reduce risk Amiodarone is a uniquely effective antiarrhythmic drug and, in addition, has the virtue of not causing very much proarrhythmia. On the negative side, it has complex pharmacokinetic properties (its half-life is between 30 and 100 days, and it does not achieve its peak efﬁcacy until it has been loaded for several weeks) and it has an extraordinarily impressive side-effect proﬁle (refer to Table 3.4). Because amiodarone must be administered for weeks before it becomes fully effective, and because, when it is discontinued, measurable amounts of amiodarone will be present in patients’ serum for a very long time, the drug is most often used empirically. Still, despite these drawbacks, its relative efﬁcacy leads electrophysiologists to using amiodarone fairly often. Several RCTs have now tested the hypothesis that empiric treatment with amiodarone is an adequate method of reducing the risk of sudden death in high-risk patients. Some of the more important studies that have examined this question are listed in Table 7.6. The bottom line is that, while amiodarone may improve mortality in some subsets of patients (a conclusion that has by no means been ﬁrmly established), it is not nearly as effective as the ICD. The use of amiodarone in high-risk patients should generally be limited to those who are not eligible for (or refuse) the ICD or as adjunctive therapy to an ICD in order to reduce the frequency of recurrent arrhythmias. 3) Ablation of reentrant foci is an effective way of treating some patients with ventricular tachycardia Because ablation can eliminate the reentrant substrate for ventricular arrhythmias, for patients whose ventricular tachycardia is suitable, ablation should be strongly considered as a treatment option. Unfortunately, only a tiny minority of patients with ventricular arrhythmias are currently good candidates for this approach. Transcatheter ablation of ventricular tachycardia will be discussed in Chapter 8. 4) In the great majority of high-risk patients, the ICD is the only treatment that reliably reduces the risk of death from ventricular arrhythmias The ICD automatically and reliably terminates the ventricular tachyarrhythmias responsible for sudden death. Except for those few cases in which ablation is a good option, no other therapy approaches the level of efﬁcacy achieved with the ICD. Indeed, when deciding on the

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Table 7.6 Randomized Clinical Trials with Amiodarone. This table summarizes the major clinical trials using amiodarone empirically in different groups of patients at increased risk for sudden death from ventricular arrhythmias. There is no evidence of a survival beneﬁt with amiodarone in patients with ischemic heart disease. While two earlier trials (GESICA and CHF-STAT) showed a trend toward beneﬁt in patients with non-ischemic cardiomyopathy, the much larger SCH-HeFT trial subsequently revealed no such trend. Study

Patient Population

Randomization

Results

GESICA1

516 pts, NYHA Class II/IV, cardiac enlargement

Amiodarone vs. placebo

CHF-STAT 2

674 pts, LVEF < 0.4, complex ectopy, cardiac enlargement

Amiodarone vs. placebo

CAMIAT3

1202 MI survivors, complex ectopy 1500 MI survivors, LVEF < 0.4 2521 pts, LVEF ≤ 0.35, NYHA class II/III

Amiodarone vs. placebo Amiodarone vs. placebo ICD vs. amiodarone vs. conventional therapy

Signiﬁcant survival beneﬁt with amiodarone at 13 months (33.5% vs 41.4%) No signiﬁcant survival beneﬁt, but pts with non-ischemic cardiomyopathy showed trend toward amiodarone beneﬁt No signiﬁcant survival beneﬁt No signiﬁcant survival beneﬁt No reduction in mortality with amiodarone; signiﬁcant survival beneﬁt with ICD

EMIAT4 SCD-HeFT5

GESICA, Study Group on Survival of Heart Failure in Argentina; CHF-STAT, Survival Trial of Antiarrhythmic Therapy in Congestive Heart Failure; CAMIAT, Canadian Amiodarone Myocardial Infarction Trial; EMIAT, European Myocardial Infarction Trial; SCD-HeFT, Sudden Cardiac Death in Heart Failure Trial; LVEF, left ventricular ejection fraction; MI, myocardial infarction; NYHA, New York Heart Association Functional Class; pts, patients. 1 — Doval HC, et al. Lancet 1994; 344:493 2 — Singh SN, et al. N Engl J Med 1995; 333:77 3 — Cairns JA, et al. Lancet 1997; 349:675 4 — Julian DG, et al. Lancet 1997; 349:667 5 — Bardy GH, et al. N Engl J Med 2005; 352:225

best therapy for a patient at high risk of sudden cardiac death, the main question is typically not whether the ICD will be effective, but instead whether one is “allowed” to use the ICD in that particular patient. Which leads us to the real question regarding the treatment of ventricular arrhythmias: When is it OK to use the ICD?

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The evidence-based approach to using the ICD

Through the 1980s, many electrophysiologists never questioned the usefulness of the ICD, a therapy whose effectiveness in patients who had recurrent ventricular tachyarrhythmias was both obvious and dramatic. Indeed, ICDs were so clearly effective that when voices were ﬁnally raised demanding randomized trials to prove the efﬁcacy of ICDs in cardiac arrest survivors, some electrophysiologists considered the proposal to be misguided. After all, they reasoned, nobody was insisting on an RCT to prove the beneﬁts of surgery for acute appendicitis — and the efﬁcacy of the ICD was every bit as dramatic and obvious as that of an appendectomy. Besides, such a trial would require doctors to randomize half of the enrolled cardiac arrest survivors to some clearly inferior therapy, thus placing them in mortal peril. We just couldn’t do that, could we? These electrophysiologists were naïve. By the late 1980s, nearly everyone embraced the notion that modern medicine must always be evidence-based, meaning that no new therapy (at least, no expensive new therapy) should ever again see the light of day without a body of evidence gathered from RCTs to support it. Evidence-based medicine was (and is) universally embraced by scientists, the medical community, and society, and the requirement for RCTs therefore trumped any other considerations. Thus, a series of randomized trials with the ICD was embarked upon. Initially, secondary prevention trials were performed in patients presenting with sustained ventricular tachyarrhythmias (that is, in patients who had been routinely receiving the ICD up to that point). Then, primary prevention trials were performed in various subsets of patients with a high risk of sudden death, but who had not yet developed such arrhythmias. As the results of these various RCTs having become available, the indications for the ICD have evolved accordingly. In keeping with the tenets of evidence-based medicine, the formal indications for ICD usage (as determined by professional organizations and the FDA) generally follow the speciﬁc design of the RCTs that justify those indications. To the extent that RCTs measuring the efﬁcacy of ICDs entail complexity in their designs, that complexity has been more or less directly translated into the resulting clinical indications. Secondary prevention trials By the mid-1990s and to the satisfaction of virtually everybody, results from three RCTs ﬁnally proved that therapy with the ICD did indeed signiﬁcantly prolong the survival of patients presenting with sustained ventricular tachyarrhythmias, as compared to other therapies (most

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speciﬁcally, amiodarone). See Table 7.7. Thankfully, the designs of these studies were relatively straightforward, and so are the subsequent indications. The ICD is now generally recognized as the treatment of choice for patients presenting with sustained ventricular tachyarrhythmias. Primary prevention trials While the secondary prevention trials with the ICD were aimed at conﬁrming the correctness of ICD usage in patients with manifest ventricular arrhythmias, the primary prevention trials have been aimed instead at testing the ICD in high-risk patients who have not yet had sustained ventricular arrhythmias. As one might predict, the designs of these studies (and therefore resulting ICD indications) have been much less straightforward than for the secondary prevention trials. Table 7.8 lists the major primary prevention trials that have affected (or will soon start affecting) indications for the ICD and their most relevant design features. MADIT I (Multicenter Automatic Deﬁbrillation Implantation Trial) was the ﬁrst primary prevention trial to be completed. In this study, patients with prior myocardial infarctions, left ventricular ejection

Table 7.7 Secondary Prevention Trials with the ICD. This table summarizes the three major randomized clinical trials conducted with the ICD in patients presenting with sustained ventricular tachyarrhythmias (i.e., the secondary prevention trials). These trials conﬁrmed the effectiveness of the ICD in patients presenting with lifethreatening, sustained ventricular tachyarrhythmias. Study

Patient population

Randomization

Results

AVID1

1016 pts with lifethreatening sustained VT/VF 288 survivors of cardiac arrest

ICD vs. amiodarone or sotalol

Survival beneﬁt with ICD

ICD vs. one of three drug treatment arms ICD vs. amiodarone

Survival beneﬁt with ICD

CASH2

CIDS3

659 pts with sustained VT/VF

Trend toward survival beneﬁt with ICD

AVID, Antiarrhythmics vs. Implantable Deﬁbrillators; CASH, Cardiac Arrest Study Hamburg; CIDS, Canadian Implantable Deﬁbrillator Study; ICD, implantable cardioverter–deﬁbrillator; pts, patients; VT/VF, ventricular tachycardia or ventricular ﬁbrillation. 1 — The Antiarrhythmics versus Implantable Deﬁbrillators (AVID) Investigators. N Engl J Med 1997; 337:1576 2 — Kuck KH, et al. Circulation 2000; 102:748 3 — Connolly SJ, et al. Circulation 2000; 101:1297

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Table 7.8 Primary Prevention Trials with the ICD. This table summarizes the major randomized clinical trials conducted with the ICD in patients with an increased risk of sudden death, but who have never experienced sustained ventricular tachyarrhythmias (i.e., the primary prevention trials). Each of these trials except DINAMIT showed a survival beneﬁt with the ICD. Owing to the varied subsets of patients entered into these trials, the resulting indications for the ICD are also somewhat complicated. See text. Study

Patient population

Randomization

Results

MADIT I1

196 MI survivors, NSVT, LVEF < 0.35, inducible VT, failed drug trial 704 MI survivors, NSVT, LVEF ≤ 0.4, inducible VT 1232 MI survivors, LVEF ≤ 0.3 2521 pts, LVEF ≤ 0.35, NYHA class II/III 674 pts, recent acute MI, LVEF ≤ 0.35, sympathetic overdrive

ICD vs. drug (mainly amiodarone)

Survival beneﬁt with ICD

No therapy vs. EPguided therapy

Survival beneﬁt in EP-guided therapy pts who received ICD Survival beneﬁt with ICD

MUSTT 2

MADIT II3 SCDHeFT4 DINAMIT5

ICD vs. conventional therapy ICD vs. amiodarone vs. conventional therapy ICD vs. conventional therapy

Survival beneﬁt with ICD; none with amiodarone Reduced arrhythmic deaths with ICD, but no overall survival beneﬁt

MADIT, Multicenter Automatic Deﬁbrillator Implantation Trial; MUSTT, Multicenter Unsustained Tachycardia Trial; SCD-HeFT, Sudden Cardiac Death in Heart Failure Trial; DINAMIT, Deﬁbrillator in Acute Myocardial Infarction Trial; EP, electrophysiology study; ICD, implantable cardioverter–deﬁbrillator; LVEF, left ventricular ejection fraction; MI, myocardial infarction; NSVT, nonsustained ventricular tachycardia; NYHA, New York Heart Association Functional Class; VT, ventricular tachycardia. 1 — Moss AJ, et al. N Engl J Med 1996; 335:1933 2 — Buxton AE, et al. N Engl J Med 1999; 341:1882 3 — Moss AJ, et al. N Engl J Med 2002; 346:877 4 — Bardy GH, et al. N Engl J Med 2005; 352:225 5 — Hohnloser SH, et al. N Engl J Med 2004; 351:2481

fractions of less than 0.35, spontaneous nonsustained ventricular tachycardia, and inducible sustained ventricular tachycardia that was not suppressed with drug testing, were randomized to receive either the ICD or the “best” antiarrhythmic drug therapy (in most cases, amiodarone). At the end of the trial, patients randomized to the ICD had signiﬁcantly improved overall survival. Subsequently, ICD indications were expanded to include patients who met all the MADIT I requirements (including electrophysiologic testing and at least one drug trial).

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MUSTT (Multicenter Unsustained Tachycardia Trial) was even more complex in design than MADIT I, and it was in fact not speciﬁcally designed as an ICD trial at all. But for our purposes, this trial can be thought of as being similar to MADIT I, except that it was more liberal in terms of its ejection fraction entrance criterion (patients were allowed into MUSTT with ejection fractions of less than 0.4). In this trial, the ICD again signiﬁcantly improved survival. MADIT II randomized patients with prior myocardial infarctions and left ventricular ejection fractions of less than or equal to 0.3 to either ICDs or conventional medical therapy. The requirements for nonsustained ventricular tachycardia and electrophysiologic testing were dropped in this trial. The results of MADIT II showed the group receiving ICDs having signiﬁcantly improved survival. SCD-HeFT (Sudden Cardiac Death in Heart Failure Trial) enrolled patients with heart failure due to either prior myocardial infarction or nonischemic cardiomyopathy. (This is the ﬁrst primary prevention trial to include nonischemic patients.) Enrollees were required to have left ventricular ejection fractions of less than or equal to 0.35 and NYHA Class II or III heart failure. They were randomized to ICD implantation, empiric amiodarone or placebo. At the end of the trial, the ICD produced a signiﬁcant reduction in overall mortality compared to either amiodarone or placebo, while amiodarone itself offered no survival beneﬁt as compared to placebo. DINAMIT (Deﬁbrillator in Acute Myocardial Infarction Trial) randomized patients to receive either an ICD or conventional medical therapy 18 days on average after an acute myocardial infarction. All patients had left ventricular ejection fractions of less than or equal to 0.35 and evidence of sympathetic over-stimulation (either reduced heart rate variability or an increased resting heart rate) but no overt congestive heart failure. The ICD reduced arrhythmic death by 50% but did not reduce overall mortality. The “excess” in non-sudden deaths in the ICD group — deaths that cancelled out the reduction in arrhythmic deaths — were due to pump failure and mainly occurred in patients who earlier had been rescued from arrhythmic death by their ICDs. The conclusion generally drawn from DINAMIT is that any decision on implanting an ICD should be delayed for 4–6 weeks following an acute myocardial infarction, in order for patients who have impending pump failure to declare themselves. It is noteworthy, however, that all patients enrolled in this study had sympathetic overdrive. Given that a rapid resting heart rate is, prognostically, the worst heart rhythm one can have after a heart attack, it is likely that DINAMIT selected patients who had a particularly high risk of developing pump failure as

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their hearts remodeled. Patients who were similar but with normal resting heart rates, well might have enjoyed an overall survival beneﬁt with the ICD — but this study did not enroll such patients, so no conclusions about them can be drawn. The DINAMIT study provides a very nice illustration of the Axiom of Overall ICD Survival (see below.) Evidence-based indications for the ICD So, after collecting all this evidence from RCTs, where do we stand? Regarding patients presenting with sustained ventricular tachyarrhythmias, the answer is simple. These patients generally ought to receive the ICD. It gets a bit more complicated when considering high-risk patients who have not yet had sustained ventricular arrhythmias (i.e., primary prevention patients). Indeed, the ICD industry, the professional organizations, and the FDA and CMS are almost continually arguing about and re-negotiating ICD indications, based on the latest available trial results. Given the “rules” of evidence-based medicine, however, indications for using the ICD for the primary prevention of sudden death seem to look something like the following. You can get an ICD: 1 . . . if you have an ejection fraction ≤0.35 from a cardiomyopathy that is either ischemic or nonischemic in origin, have not had an acute myocardial infarction within 4–6 weeks*, and have NYHA Class II /III heart failure (from SCD-HeFT); or 2 . . . if you do not have NYHA Class II /III heart failure, but have had a prior myocardial infarction more than 4–6 weeks ago* and an ejection fraction ≤0.3 (from MADIT II); or 3 . . . if you do not meet criteria 1 or 2, but have had a prior myocardial infarction more than 4–6 weeks ago*, an ejection fraction of <0.4 (from MUSTT) or <0.35 (from MADIT I), nonsustained ventricular tachycardia, and inducible sustained ventricular tachycardia that is not suppressed with drug testing. Why, in the case of the ICD, the evidence-based approach might not be the best alternative

The widespread adoption of RCTs has been one of the major advances in health care over the past few decades. The scientiﬁc rigor of welldesigned RCTs has revolutionized our management of acute myocardial

*The imperative to wait 4–6 weeks after an acute myocardial infarction comes mainly from DINAMIT.

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infarction, heart failure, and hypertension; not to mention cancer, stroke, arthritis, and countless other health problems — much to the beneﬁt of millions of patients. Such advances would have been impossible by any other method. The unassailable theoretical advantages of the RCT, added to the remarkable clinical successes produced by its application, have led to a situation where RCTs are not merely strongly urged as a methodology for proving a medical therapy — they are absolutely insisted upon. While most reasonable scientists will agree that there are circumstances under which conducting an RCT is unnecessary, impracticable, or unethical, some will not. These latter have created an irony, for their unyielding insistence upon RCTs for the sake of scientiﬁc purity has become dogma. At the risk of being heretical, then, the author respectfully submits that the expansion of indications for the ICD is one of the rare instances in which RCTs are not necessary in order to achieve scientiﬁc rigor, and that there may be a better way of getting the answer everybody claims to be seeking. Drawbacks of randomized ICD trials The purpose of primary prevention trials with the ICD is to assess whether it is appropriate to expand ICD indications to cover high-risk patients who are not now eligible for the device. The methodology employed invariably identiﬁes a subset of patients who are at increased risk for sudden death — and designs an RCT aimed at that particular subset. As we have seen, the indications for ICD usage at any given time amount to a patchwork of the various subsets of high-risk patients that have been studied in one successful RCT or another. Aside from being confusing, this approach is hugely expensive and time-consuming. Several of the major trials cited above have taken three to ﬁve years to complete. Once an RCT is completed, the data analysis and publication in a peer-reviewed journal, followed by formal consideration of new indications by advisory and regulatory organizations, can add another two years to the process — time during which affected patients must wait before reaping the beneﬁts of the RCT. Overall, adding another subset of high-risk patients to the list of subsets eligible for the ICD can consume seven or eight years, and from $50 million to $100 million dollars. Because the great bulk of this expense is borne by ICD manufacturers, it is hard for most of us to get exercised about it, at least on ﬁrst consideration. It turns out, however, that this system is one of the major

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factors keeping the cost of ICDs high, and (for this and other reasons) is an inefﬁcient way of making this therapy available to patients that would beneﬁt from it. Indeed, after 15 years of applying the evidencebased paradigm to ICD usage, only a small proportion of high-risk patients are eligible for ICDs, and it is inconceivable that the majority of these patients will ever be able to have an ICD under such a system. If our long-term goal is to substantially reduce the hundreds of thousands of sudden deaths that occur each year, our current methods will never get us there. The axiom of overall ICD survival There is an alternative to the RCT for legitimately expanding the use of the ICD. This alternative is available because of the unique and unquestioned efﬁcacy of the ICD itself — that is, the ICD is extraordinarily effective at doing exactly what it was designed to do; namely, to automatically detect and terminate spontaneous episodes of ventricular tachyarrhythmias. It is thus a given that the ICD will nearly eliminate the risk of purely arrhythmic sudden death. Because of this given, we can deﬁne an Axiom of Overall ICD Survival, to wit: Over any given period of time, the ICD will signiﬁcantly prolong the overall survival of a population of patients, as long as the risk of arrhythmic death in that population is sufﬁciently high and the risk of death from all other causes is sufﬁciently low.

The Axiom of Overall ICD Survival means that if we want to determine whether using an ICD in a certain population of patients will signiﬁcantly prolong survival, all we need to know is the risk of sudden death in that population, and the risk of death from all other causes. This kind of information does not require an RCT; it can often be estimated from an epidemiological database, such as the Framingham study. So, for instance, in patients with structurally normal hearts but with a history of syncope-producing ventricular tachycardia (such as patients with the Brugada syndrome), we don’t need an RCT to understand that the ICD will prolong overall survival. In contrast, in patients with a history of sustained ventricular tachyarrhythmias, but who also have metastatic lung cancer, we know without the results of an RCT that implanting ICDs will not yield a meaningful survival beneﬁt. These are extreme and obvious examples of how the Axiom can help us decide whether using ICDs makes sense without the expense and inconvenience of conducting an RCT. For a more relevant example, consider a population of middle-aged patients with preserved ventricular

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function but who are obese, have metabolic syndrome, and have strong family histories of premature cardiac disease. We have enough information from epidemiologic studies to know that, over a period of 5–10 years, these individuals will have a substantially increased risk of both sudden arrhythmic death and non-sudden cardiac death — and we can quantify those risks. From the Axiom, we could estimate right now, if we chose, the degree of survival beneﬁt that we could expect from using the ICD. Conducting an RCT would be another way of estimating the ICD-related survival beneﬁt in these patients, but clearly the RCT method is far costlier and more time-consuming, and (given the vagaries of and compromises typically made in designing RCTs) might very well fail to yield a “better” estimate. While in almost every other case, RCTs (despite inherent problems in their design) are the best possible approach to estimating the beneﬁt of a therapy, in the singular case of ICDs, thanks to the Axiom, there is a quicker, more efﬁcient way of getting that answer. Whether we estimate the survival beneﬁt with the ICD from an RCT or the Axiom, however, we are still left with a big problem: Given some estimated degree of survival beneﬁt imparted by the ICD, is that beneﬁt “sufﬁcient” to justify the expense? For fundamentally, whether or not to use the ICD in high-risk patients is much less a matter of estimating beneﬁt, and much more a matter of economics. Managing the cost of ICDs The cost — what we ought to be willing to spend to prolong life with the ICD — is the crux of the matter. After all, if we know that the ICD virtually eliminates sudden arrhythmic death, and if we know that we can identify the majority of patients at increased risk for sudden death, then why don’t we just use the ICD in all of them? Obviously, it is because of the expense this would entail. To place this undeniable fact into a different formulation, but for the expense we would offer an ICD to almost any patient we knew to have a signiﬁcantly increased risk of sudden death. This formulation is the “but for” test; a test used by medical ethicists to identify whether health care rationing is taking place. The fact that the “but for” test applies to our usage of the ICD explains a lot. It tells us that we are indeed rationing the ICD. Further, it suggests that one major reason we continue to insist on RCTs, despite the fact that the Axiom makes RCTs unnecessary, may be that requiring RCTs presents a huge hurdle to the expansion of ICD usage, and thus serves as a powerful mechanism for rationing.

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The foregoing is not to criticize the rationing itself. The fact is that we have no alternative but to ration the ICD; at least, until the price of these devices drops dramatically. However, the means we have chosen for implementing the necessary rationing — the RCT pathway — is not only inefﬁcient but counterproductive in the long run. We have seen that RCTs are very expensive and very time consuming. While this helps to limit the number of RCTs and thus limits the expansion of ICD usage (and thus achieves rationing), it is also a driving force for keeping the cost of ICDs themselves high. Indeed, it is difﬁcult to imagine a scenario under the “RCT paradigm” that will allow a dramatic reduction in the cost of ICDs. As long as carving out another subset of high-risk patients for an ICD indication requires another expensive RCT, manufacturers of ICDs will need to keep their prices high in order to recoup their investment — and to fund the next RCT. An easier, more equitable, more honest, and more scientiﬁcally legitimate approach than “rationing by RCT” would be to openly admit that we need to ration the ICD due to its expense, and then to declare how much we are willing to spend to prolong survival with ICDs. Having made such a declaration, all we would need to do to determine which individuals can receive ICDs is to do the appropriate calculations. The Axiom of Overall ICD Survival shows us how to perform those calculations, as illustrated in Tables 7.9 and 7.10. Given a well-deﬁned subset of patients, we would merely enter four simple variables into this spreadsheet: The annual risk of sudden death, the annual risk of death from all other causes, the cost of implanting an ICD, and the longevity of the ICD chosen. Table 7.9 shows results for a subset of patients whose annual risk of sudden death is 7%, the annual risk of non-sudden death is 5%, and the cost of a 5-year ICD is $30,000. The spreadsheet estimates the cost per life-year saved as about $42,000. In contrast, Table 7.10 shows the calculations for patients with a 10% yearly risk of sudden death but a 33% yearly risk of non-sudden death, using the same ICD. Here, the cost per life-year saved is about $97,000. To determine whether an ICD is justiﬁed, we simply need to decide how much we are willing to spend to save one life-year. If we make our cut-off the traditional $50,000 per life-year saved, the patient in the ﬁrst example could receive an ICD; the patient in the second example could not. Here is where it gets interesting. Consider how the manufacturers of ICDs would respond to such a methodology. For the ﬁrst time, the price of ICDs would directly determine which patients could receive a device, and which manufacturer’s device they could receive. The lower the price and the greater the longevity of an ICD, the greater the number of patients who could receive one, and the more devices would be sold.

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Table 7.9 Calculating the Projected Cost per Life-Year Saved with an ICD (1). This spreadsheet, based on the Axiom of Overall ICD survival (see text), projects the cost per life-year saved by implanting ICDs in 100 patients, assuming the following variables: Yearly risk of sudden death for these patients is 7%. Yearly risk of death from other causes is 5%. Cost of the ICD being used is $30,000. Projected longevity of ICD being used is 5 years. From these four variables, the projected cost per life-year saved is $41,600. Yearly risk of sudden death Yearly risk of nonsudden death Cost of ICD Longevity of ICD

# pts alive at beginning of year # projected nonsudden deaths # projected additional sudden deaths # projected total deaths without ICD # projected deaths with ICD Pts saved this year by ICD Saved pts from last year still alive Total saved pts still alive Total life-years saved this year Cumulative life-years saved # pts projected alive at end of year

7% 5% $30,000 5 years

Year 1

Year 2

Year 3

Year 4

Year 5

100 5 6.65 11.65 5

95 4.75 6.32 11.07 4.75

90.25 4.51 6.00 10.51 4.51

85.74 4.29 5.70 9.99 4.29

81.45 4.07 5.42 9.49 4.07

6.65 0 6.65 3.33 3.33 95

6.32 6.32 12.64 9.48 12.8 90.25

6.00 12.00 18.00 15.00 27.81 85.74

5.70 17.10 22.81 19.96 47.76 81.45

5.42 21.67 27.08 24.37 72.13 77.38

Total life-years saved Life-years saved per pt Cost of ICD Cost per life-year saved

72.13 0.72 $30,000 $41,600

ICD, implantable cardioverter–deﬁbrillator; pts, patients.

(Another way of looking at it is that as the overall price of an ICD comes down, the “indications” for that ICD would immediately and automatically expand proportionally.) Real price competition would take place for the ﬁrst time. This competition would also change the way technology is applied. Technology would no longer be recruited by ICD manufacturers for the purpose of adding more bells and whistles to ever-fancier ICDs, but instead for the purpose of building simpler, longer-lasting, reliable devices, as cheaply as possible. Market forces would be unleashed in a more cost-effective direction. Eventually, most

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Table 7.10 Calculating the Projected Cost per Life-Year Saved with an ICD (2). Table 7.10 projects the cost per life-year saved by implanting ICDs in 100 patients with the following variables: Yearly risk of sudden death is 10%. Yearly risk of death from other causes is 33%. Cost of the ICD is $30,000. Projected longevity of ICD is 5 years. From these four variables, the projected cost per life-year saved is $96,700. As long as one can make a reasonable estimate on the four required variables for a given population of patients and a given ICD, a randomized clinical trial is not necessary for estimating the cost per life-year saved. Yearly risk of sudden death Yearly risk of nonsudden death Cost of ICD Longevity of ICD

# pts alive at beginning of year # projected nonsudden deaths # projected additional sudden deaths # projected total deaths without ICD # projected deaths with ICD Pts saved this year by ICD Saved pts from last year still alive Total saved pts still alive Total life-years saved this year Cumulative life-years saved # pts projected alive at end of year

10% 33% $30,000 5 years

Year 1

Year 2

Year 3

Year 4

Year 5

100 33 6.7 39.7 33

67 22.11 4.49 26.60 22.11

44.89 14.81 3.01 17.82 14.81

30.08 9.93 2.01 11.94 9.93

20.15 6.65 1.35 8.00 6.65

4.49 4.49 8.98 6.74 10.08 44.89

3.01 6.02 9.02 7.52 17.60 30.08

2.02 6.05 8.06 7.05 24.66 20.15

1.35 5.40 6.75 6.08 30.73 13.50

6.7 0 6.7 3.35 3.35 67

Total life-years saved Life-years saved per pt Cost of ICD Cost per life-year saved

30.73 0.31 $30,000 $96,700

ICD, implantable cardioverter–deﬁbrillator; pts, patients.

individuals at increased risk for sudden death would have access to a new breed of simple and inexpensive, yet highly reliable ICDs. By rationing ICDs openly, guided by the Axiom of Overall ICD Survival, not only would we ration more fairly and more equitably than we are today, but also we would end up driving the cost of ICDs down, stimulating innovation in a new direction, and ultimately, conducting less rationing, not more. None of this, of course, is likely to happen since it would require doctors, payers, and federal agencies to publicly admit that we are ration-

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ing health care. So, for the foreseeable future, preventing sudden death will continue to boil down to ﬁguring out whether we are able to shoehorn that high-risk patient sitting in front of us into one of the RCTsanctioned subsets.

Fig. 7.15 Summary of evidence-based strategy for treating high-risk Patients. This treatment strategy is derived from the results of the randomized trials discussed in Chapter 7. See text for details. “Conventional” antiarrhythmic therapy consists of any arrhythmia therapy the physician chooses, short of an ICD. ICD1, evidence base for this treatment node comes from the secondary prevention trials with the ICD; ICD2, evidence base for this treatment node comes from SCD-HeFT; ICD3, evidence base for this treatment node comes from MADIT II; ICD4, evidence base for this treatment node comes from MADIT I (for ejection fractions <0.35) and MUSTT (for ejection fractions <0.4). Note: For any primary prevention indication, the general consensus is that ICDs should not be implanted for 4–6 weeks following an acute myocardial infarction (from DINAMIT). EF, ejection fraction; ICD, implantable cardioverter–deﬁbrillator; NYHA, New York Heart Association Functional Class; MI, myocardial infarction; VT/VF, ventricular tachycardia or ventricular ﬁbrillation.

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Summary of an evidence-based treatment strategy for high-risk patients

Figure 7.15 outlines a treatment strategy for patients who are at a high risk of sudden death from ventricular tachyarrhythmias, as derived from the RCTs discussed in this chapter. Under this strategy, two general forms of therapy are available: The ICD, and “conventional” arrhythmia therapy. Such conventional arrhythmia therapy would consist of whichever treatment the physician chooses short of the ICD, possibly including empiric amiodarone, antiarrhythmic drugs selected by serial drug testing or some other methodology, or no speciﬁc antiarrhythmic therapy. It is assumed that all patients will receive any indicated conventional cardiac therapy (such as β blockers, ACE inhibitors, and ischemia control) as well as any necessary risk factor modiﬁcation, whether they receive the ICD or not. Under this treatment strategy, patients presenting with sustained ventricular tachycardia or ventricular ﬁbrillation generally are offered the ICD. All other high-risk patients should be evaluated to determine whether they fall into one of the ICD-sanctioned subsets as derived from the primary prevention trials discussed above. Those who have either ischemic or nonischemic cardiomyopathy with ejection fractions of less than or equal to 0.35 and NYHA Class II or III heart failure, but have not had a myocardial infarction within the past 4–6 weeks, should be offered an ICD. The evidence for this treatment node comes from SCD-HeFT. Any patients with nonischemic cardiomyopathy who do not meet the SCD-HeFT criteria should be offered “conventional” therapy. Patients with ischemic heart disease not meeting SCD-HeFT criteria may receive an ICD if they have not had myocardial infarctions within the past 4–6 weeks, have ejection fractions of less than or equal to 0.3, and are NYHA Class I. The evidence for this treatment node comes from MADIT II. If patients with ischemic heart disease fail to meet either the SCDHeFT or the MADIT II criteria, they may still be eligible for the ICD if they have not had myocardial infarctions within the past 4–6 weeks, have ejection fractions of less than 0.35 (or possibly less than 0.4) and also have nonsustained ventricular tachycardia, and, when then sent for electrophysiologic testing, are found to have inducible ventricular tachycardia that is not suppressed during at least one trial with an antiarrhythmic drug. This treatment node is supported by MADIT I (for ejection fractions of less than 0.35) and by MUSTT (for ejection fractions of less than 0.4).

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All other patients will be eligible for “conventional” treatment only. Note 1: The imperative to wait 4–6 weeks following an acute myocardial infarction before implanting an ICD for the primary prevention of sudden death comes mainly from DINAMIT. Note 2: The only NYHA Class I patients with a primary prevention indication for an ICD are those who meet MADIT II criteria (i.e., patients with prior MI who have ejection fractions of less than 0.3). Very few patients with these low ejection fractions can be expected to be in NYHA Class I. Note 3: Recently, the Centers for Medicare & Medicaid Services (CMS) ruled that patients who meet CMS requirements for cardiac resynchronization therapy (CRT) and are NYHA Class IV can receive a CRT device that also provides deﬁbrillation therapy. This is the only group of patients in NYHA Class IV who currently has an indication for implantable deﬁbrillation therapy; the rationale here is that Class IV patients who receive CRT therapy often experience a signiﬁcant improvement in their functional class — and would thus ﬁnd themselves eligible for an ICD a few weeks or months after receiving CRT. (CRT devices are discussed in Chapter 9.)

CHAPTER 8

Transcatheter Ablation: Therapeutic Electrophysiology

Over the past two decades, the most important advance in the ﬁeld of electrophysiology has been the rapid transformation of the electrophysiology study from a largely diagnostic procedure to a largely therapeutic one. Many cardiac arrhythmias that formerly required the use of potentially toxic drugs or cardiac surgery now can be routinely cured (or at least palliated) in the electrophysiology laboratory by means of transcatheter ablation techniques. The basic idea behind transcatheter ablation is to position a catheter to a critical area within the heart, and to apply damaging energy through the catheter in order to create a discrete scar. Strategically placed scar tissue can disrupt the pathways necessary for pathologic tachyarrhythmias, since it is electrically inert. In this chapter, we will brieﬂy review the techniques used to ablate cardiac arrhythmias in the electrophysiology laboratory and the present-day applications of those techniques.

The technology of transcatheter ablation Successful catheter ablation requires three things. First, it requires a thorough understanding of the arrhythmia being treated — speciﬁcally, it requires a precise understanding of the location and physiology of the electrical pathways involved. Second, it requires an understanding of the cardiac anatomy associated with those pathways. Finally, it requires the technology to enable the precise positioning of a catheter and to create the right kind of lesion at a critical location within the pathway. The rapid advance of transcatheter ablation as a therapeutic technique has hinged on the steady progression in all three of these requirements. We will begin by brieﬂy reviewing the technology of lesion generation, and then we will survey the electrophysiology and anatomy of the arrhythmias that have proven amenable to transcatheter ablation. 211

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Direct current shocks

The use of direct current (DC) shocks for transcatheter ablation is now mainly of historical interest, as DC energy has been entirely supplanted for this use by radiofrequency (RF) energy. From the ﬁrst successful ablation in a human in 1982 until approximately 1989, however, DC shocks were the most commonly used energy source for performing transcatheter ablation. To ablate with DC energy, a standard electrode catheter is connected to a conventional deﬁbrillator, and a shock is delivered to the distal electrode of the catheter, using a surface electrode as the energy sink. DC shocks delivered in this way generate very high voltages (2000–4000 V) and high currents at the catheter tip. The temperature of the tip electrode instantaneously rises to thousands of degrees Celsius. The resultant vaporization of blood creates a virtual explosion within the heart, manifested by a rapidly expanding and collapsing incandescent gas globe that generates instantaneous pressures of up to 70 lb/in2 and produces a ﬂash of light and a disquieting popping noise. Thus, transcatheter DC shocks result in several forms of potentially damaging energy — light, heat, pressure, and electrical current. The only “useful” damage created by DC shocks is thought to result from the electrical current; all the other forms of energy tend only to increase the possibility of complications. The extent of the lesions created by DC energy is related to the amount of energy used. With energies in excess of 250 J, transmural lesions of 2–4 cm2 are common. Unfortunately, the periphery of the lesions created with DC shocks is often patchy — and therefore potentially arrhythmogenic. Because of the traumatic nature of intracardiac DC shocks and because of the nonideal lesions created, DC energy proved to be of limited utility. Ablation with DC shocks was largely limited to ablation of the His bundle to produce complete heart block. Meanwhile, researchers sought alternative means of creating intracardiac lesions that would be less dangerous and more effective. Radiofrequency (RF) energy

As it turned out, such a means was readily available. Radiofrequency (RF) energy had been used for many years in operating rooms (in the form of Bovie machines) to cauterize small bleeding vessels within the surgical wound. It wasn’t long before electrophysiologists recognized that attaching an RF generator to an electrode catheter would permit the creation of a discrete, well-demarcated intracardiac lesion.

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RF energy consists of alternating current with a frequency range of 100 kHz to 1.5 MHz. In the electrophysiology lab, relatively low frequencies are used in order to avoid the sparking seen with the higher frequencies used in the operating suite. The RF current ﬂow causes localized heating at the tip of the catheter and leads to desiccation and coagulation necrosis of the underlying tissue. The voltage created during RF ablation is relatively low (40–60 V), thus avoiding the barotrauma (i.e., the explosion) seen with DC shocks. RF generators speciﬁcally designed for electrophysiology procedures are now widely available. These RF generators allow instantaneous monitoring of the energy being delivered to the cardiac tissue. The voltage, current, wattage, and impedance can be tracked, permitting the operator to carefully titrate the applied energy. In addition, some ablation systems allow monitoring of the temperature at the catheter tip, thus enabling the operator more easily to avoid coagulation of blood. (Temperatures in excess of 100°C are associated with formation of a coagulum at the catheter tip, thus dramatically decreasing the energy delivered to the target tissue.) Special catheters have also been developed for use during RF ablation procedures. These catheters come in a variety of shapes and sizes, and allow the operator to apply variable amounts of “bend” to the distal end, in order to facilitate accurate manipulation of the tip of the catheter. Ablation catheters also come equipped with enlarged tip electrodes (usually 4 mm, instead of the “standard” electrode size of 1 mm). The enlarged surface area provides for a more efﬁcient application of RF energy. RF energy has several advantages over DC shocks. First, RF energy does not produce an explosion. It can thus be applied, in judicious amounts, to thin-walled structures such as the coronary sinus and cardiac veins without producing rupture. Second, RF energy produces very little stimulation of muscle or nerve, so it can be applied without using general anesthesia. Third, because the energy applied can be titrated, graded amounts of energy can be delivered to cause partial tissue damage. Fourth, RF energy produces small, homogeneous lesions, which are less arrhythmogenic. There are also two disadvantages to the use of RF energy. First, the lesions it produces are small (4–5 mm in diameter and approximately 3 mm in depth). Extremely precise mapping is thus required in order to damage the target area sufﬁciently, and target tissue that is relatively broad or deep (e.g., a bypass tract that is located epicardially) might not be readily amenable to RF ablation. Further, the delivery of RF energy is not instantaneous. This means that stable contact between the catheter

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tip and the tissue must be maintained during the entire 5–120 seconds during which RF energy is applied. Monitoring of the impedance in the ablation system during the application of energy is helpful in ensuring adequate tissue contact. Several other kinds of energy are being developed for the transcatheter ablation of arrhythmias — including laser energy, microwave energy, and cryoenergy (i.e., freezing). While each of these forms of energy is being used clinically today in ablation procedures, and while one or more of these may end up largely supplanting RF ablation, RF energy remains by far the most commonly used method of ablating cardiac arrhythmias.

Ablation of the AV junction The original indication for transcatheter ablation was to produce complete heart block in patients with chronic atrial ﬁbrillation and persistently rapid ventricular rates. AV junction ablation with DC energy

Originally, DC shocks were used in performing transcatheter ablation of the AV junction. With this technique, the target tissue was the His bundle itself. After placing an electrode catheter in the right ventricle so that pacing could be established, the ablation catheter was used to localize the His bundle (as described in Chapter 4). Careful unipolar mapping of the His bundle was then performed to ensure that the distal electrode (i.e., the ablating electrode) was nearest the His bundle itself. The patient was then placed under general anesthesia, and a 200–400 J shock was delivered to the His bundle via the distal electrode. Figure 8.1 shows DC ablation of the His bundle in a patient with atrial ﬁbrillation. Note the slow ventricular escape rhythm following the successful ablation. DC ablation of the His bundle was successful in 85% of patients in whom it was attempted, and serious complications (despite the unsettling physics associated with intracardiac DC shocks) were remarkably uncommon. AV junction ablation with RF energy

In the early 1990s, RF energy began to supplant DC energy as the method of choice for ablating the AV junction. Aside from the fact that it is inherently safer, the major advantage of RF energy is that with RF ablation, disruption of the AV node (as opposed to the His bundle) can be performed. This more proximal ablation site generally leaves the patient

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Fig. 8.1 Ablation of the His bundle using a DC shock. (A) Two surface ECG leads and the unipolar His bundle electrogram are shown. Atrial ﬁbrillation is present. Once the position of the His catheter is optimized, the catheter is attached to a deﬁbrillator (the * indicates where the catheter has been attached to the deﬁbrillator) and a 300-J shock is delivered through the His catheter (indicated by **). (B) 30 seconds after the shock, complete heart block is present, with a slow ventricular escape mechanism.

with a more favorable escape rhythm after complete heart block is created. To perform RF ablation of the AV junction, a temporary pacemaker is ﬁrst placed into the right ventricle. The ablation catheter is then used to map the His bundle. Once the largest His deﬂection is carefully localized, the catheter is gradually withdrawn while recording from the distal (ablating) electrode, until the His and ventricular deﬂections become relatively small and the atrial deﬂection becomes relatively large. This position indicates that the catheter tip is in the region of the compact AV node. Excellent contact of the catheter tip with the cardiac tissue must be seen, and the catheter position must be entirely stable. When optimal positioning has been conﬁrmed, RF energy is applied to the tip electrode (usually 20–35 W for 30–60 seconds). Successful AV nodal ablation is often heralded by the development of an accelerated junctional tachycardia during application of the RF energy. (Hence, junctional tachycardia during RF application is a “good sign”.) If the attempt is unsuccessful, the catheter is repositioned and RF ablation repeated. In the hands of an experienced operator, RF ablation of the AV junction is possible in virtually 100% of cases, although in 5–10% of cases, a second procedure is required to assure permanent block. Occasionally, ablations of the AV junction using this technique will be unsuccessful, and in these cases ablation of the His bundle from the left ventricle may be required. Ablating the His bundle from the left ventricle is accomplished by positioning the ablation catheter just

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inferiorly to the aortic valve along the septal wall of the left ventricle. The intracardiac electrogram during left-sided ablation should show a His bundle deﬂection at least 110 msec earlier than the ventricular deﬂection. (A closer spacing between the His deﬂection and the ventricular deﬂection means that the catheter is not actually recording the His bundle, but instead is recording the left bundle branch.) A few cases of sudden death have been reported within several days of ablation of the AV junction. It is thought that these deaths are likely due to torsade de pointes, most likely provoked in susceptible patients by a sudden, relative bradycardia. The risk for this event appears to be transient, and can be avoided by pacing patients relatively rapidly (i.e., 90– 100 beats/min) for a few days to a few weeks after AV junction ablation.

Ablation of AV nodal reentrant tachycardia During the past decade, RF ablation has become the treatment of choice for AV nodal reentrant tachycardia. Successfully ablating AV nodal reentrant tachycardia has required a change in the way electrophysiologists visualize the AV node. In the past, most electrophysiologists thought of the AV node simply as a compact, button-like structure, as depicted in Figure 8.2A. It has now become apparent that the AV node behaves more as depicted in Figure 8.2B. The AV node does indeed appear to have a compact distal component (i.e., the part of the node that gives rise to the His bundle), but the more proximal portion of the AV node appears to be “diffuse”. To visualize what this means, it is helpful to imagine the course of the electrical impulse as it approaches the AV node from the atria. We have seen that the electrical impulse arises in the sinus node, and then travels across the atria in a radial fashion. Recent ﬁndings suggest that as this electrical impulse approaches the AV node, it is gathered into bands of conducting ﬁbers that coalesce into “tracts”, which in turn coalesce to form the compact AV node. At some point, the cellular electrophysiology of these coalescing tracts changes over (in what is referred to as a transition zone) from behaving like typical atrial tissue to behaving like typical AV nodal tissue. Thus, the point at which the AV node “begins” is inherently indistinct and diffuse and probably varies from patient to patient. The tracts of atrial ﬁbers that coalesce to form the AV node are illdeﬁned, and until recently were completely theoretical. It now appears, however, that (at least in patients with AV nodal reentrant tachycardia and probably in all individuals), two distinct tracts can be localized anatomically — the anterior tract (which corresponds to the fast AV nodal

Fig. 8.2 “Old” and “new” concepts of AV node anatomy and physiology. (A) The AV node as it commonly used to be conceived, namely, as a compact “button” of specialized tissue. (B) The AV node as it is currently conceptualized by electrophysiologists. In this “new” model, tracts of conducting ﬁbers coalesce to form the compact AV node. The transition from atrial electrophysiology to AV nodal electrophysiology probably occurs proximal to the compact node. Anatomists have been describing this for years, but until ablationists arrived on the scene, there seemed to be no good reason to believe them.

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pathway) and the posterior tract (which corresponds to the slow AV nodal pathway). The “classic” way of visualizing the two pathways involved in AV nodal reentrant tachycardia is seen in Figure 6.12, in which the two tracts are seen as a functional division within the button-like AV node. To visualize the dual AV nodal pathways as currently conceptualized, one must be familiar with the anatomy of Koch’s triangle (Figure 8.3). The three sides of Koch’s triangle are deﬁned by the tricuspid annulus (the portion of the annulus adjacent to the septal leaﬂet of the tricuspid valve), the tendon of Todaro, and the os of the coronary sinus. The His bundle is located at the apex of Koch’s triangle. Therefore, the major landmarks that deﬁne Koch’s triangle (the tricuspid valve, the os of the

Fig. 8.3 The triangle of Koch. Also long described by anatomists and long ignored by electrophysiologists, Koch’s triangle has become vitally important in performing transcatheter ablations. Koch’s triangle is deﬁned posteriorly by the os of the coronary sinus. The apex of the triangle is deﬁned anteriorly by the His bundle. The tendon of Todaro and the tricuspid valve annulus comprise the other two sides of the triangle. In the electrophysiology laboratory, the landmarks of Koch’s triangle are identiﬁed by one catheter recording the His deﬂection and by a second catheter placed in the os of the coronary sinus. Koch’s triangle lies between these two catheters.

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coronary sinus, and the His bundle) are readily identiﬁable during electrophysiologic testing. It is important to recognize that the apex of Koch’s triangle (i.e., the angle where the AV node and His bundle reside) is an anterior structure — in fact, the apex of Koch’s triangle deﬁnes the anterior aspect of the atrial septum. In contrast, the os of the coronary sinus is a posterior structure and deﬁnes the posterior portion of the atrial septum. In patients with AV nodal reentrant tachycardia, the fast and slow pathways can be visualized as two tracts of atrial ﬁbers that coalesce to form the compact AV node (Figure 8.4). The fast pathway is an anterior and superior tract of ﬁbers, located along the tendon of Todaro. The slow pathway is a posterior and inferior tract of ﬁbers, located along the tricuspid annulus near the os of the coronary sinus. Thus, the anatomic correlates of the “functional” dual AV nodal pathways have now been identiﬁed. Because the two pathways can be discretely localized, they can be discretely ablated.

Fig. 8.4 The fast and slow pathways in patients with AV nodal reentrant tachycardia, relating to Koch’s triangle. The dual AV nodal pathways seen in patients with AV nodal reentrant tachycardia have classically been considered to lie within a button-like AV node. Electrophysiologists performing radiofrequency transcatheter ablation, however, have now clearly shown that the fast and slow pathways are readily discernible and can be distinctly localized within Koch’s triangle. Both pathways appear to be located proximally to the compact AV node. The fast pathway is an anterior and superior structure and lies near the compact AV node along the tendon of Todaro. The slow pathway is a posterior and inferior structure and can usually be identiﬁed along the tricuspid annulus near the os of the coronary sinus. Because the slow pathway is farther away from the AV node than the fast pathway, the slow pathway can usually be selectively ablated without causing complete heart block.

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When the anatomy of dual AV nodal pathways was ﬁrst recognized, most attempts at curing AV nodal reentry focused on ablating the fast pathway. These attempts were generally successful, but unfortunately they yielded a relatively high incidence of complete heart block (up to 20%). The heart block most likely resulted from the fact that the fast pathway and the compact AV node are in close proximity (i.e., both structures are anterior). The ablation of AV nodal reentry in recent years has been generally accomplished by ablating the slow pathway. Since the slow pathway is posterior, it is relatively distant from the AV node, and thus ablation of this structure yields a low incidence of complete heart block (generally less than 1%). In general, two approaches are commonly used for ablation of the slow AV nodal pathway — the “mapping” approach and the anatomic approach. Both approaches begin by ﬁrst identifying the anatomic limits of Koch’s triangle, by placing one catheter in the His position and another in the os of the coronary sinus. The ablation catheter is then advanced from the femoral vein to the tricuspid annulus, near the os of the coronary sinus. With the “mapping” approach, the ablation catheter is carefully manipulated along the tricuspid annulus, searching for discrete “slow potentials” that presumably represent depolarization of the slow pathway itself (Figure 8.5). These slow potentials are located between the atrial and ventricular deﬂections in the intracardiac electrogram. Mapping of AV nodal reentrant tachycardia is thus best accomplished during sinus rhythm and not during tachycardia, so that the atrial and ventricular deﬂections during mapping remain separate and distinct. When the slow potentials are identiﬁed, an RF lesion applied to that location almost always ablates the slow pathway. With the anatomic approach to slow pathway ablation, no attempt is made to map the slow potentials. Instead, ablation sites are identiﬁed by ﬂuoroscopic means. Generally, the length of the tricuspid annulus between the os of the coronary sinus and the His bundle is visually divided into three equal sections — posterior (closest to the os of the coronary sinus), middle, and anterior (closest to the His bundle). The ablation catheter is positioned across the tricuspid valve in the posterior section and gradually withdrawn until both atrial and ventricular deﬂections are recorded, with the ventricular deﬂection larger than the atrial deﬂection. An RF lesion is made, and if the slow pathway has not been successfully ablated, the catheter is moved further anteriorly and the procedure repeated. Serial lesions are placed in each of the three sections serially, from posterior to anterior, until the slow pathway has been ablated.

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Fig. 8.5 Slow AV nodal pathway potential. Mapping of the slow pathway in patients with AV nodal reentrant tachycardia is accomplished by seeking the slow potential (SP) along the tricuspid annulus within Koch’s triangle. See text for details. A, atrial deﬂection; V, ventricular deﬂection.

Many electrophysiologists have evolved an integrated approach which begins with ablations posteriorly and moving anteriorly (as with the anatomic approach), but adding at least a brief search for slow pathway potentials within that anatomic zone prior to applying RF energy. Accelerated junctional tachycardia occurs during RF application in virtually 100% of successful slow pathway ablations. Therefore, if no tachycardia occurs after 10–15 seconds of RF application, the RF should be terminated and the catheter repositioned. If tachycardia does occur, 30–60 seconds of RF energy should be applied. Successful ablation is documented by conﬁrming that the physiology of dual AV nodal pathways is no longer present (see Chapter 6). When one or both of these techniques for slow pathway ablation are used, successful treatment of AV nodal reentrant tachycardia can be achieved in over 98% of patients, with a very low risk of producing complete heart block.

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Ablation of bypass tracts In the late 1980s, RF ablation of bypass tracts was considered a difﬁcult and somewhat mystical technique performed by only a few adventurous shamans. During the 1990s, however, it evolved to a widely available and highly effective procedure. For most patients with signiﬁcantly symptomatic or life-threatening bypass tracts, RF ablation is now the therapy of choice. Characteristics of bypass tracts

As noted in Chapter 6, bypass tracts are tiny bands of myocardial tissue that form a bridge across the AV junction, connecting atrial tissue to ventricular tissue. They can occur anywhere along the AV groove, except along the portion directly between the mitral and aortic valves. Because they are composed of bands of myocardial tissue, bypass tracts tend to exhibit the electrophysiologic features of myocardial tissue instead of AV nodal tissue; that is, their refractory periods tend to shorten instead of lengthen with decreases in cycle length, and they tend to develop second-degree block in a Mobitz II pattern instead of a Mobitz I pattern. Localization of bypass tracts begins by studying the surface ECG, and continues with intracardiac mapping. ECG localization of bypass tracts

Bypass tracts are divided into ﬁve general categories according to their location (Figure 8.6). These categories are left free wall, right free wall, posterior septal, anterior septal, and midseptal. The general approach to mapping in the electrophysiology laboratory is different for each of these categories, so it is important to have some idea as to the location of a bypass tract before the ablation procedure begins. In most cases, the surface ECG fortunately gives a very good indication of where the bypass tract is located. Table 8.1 lists the ECG criteria for grossly localizing bypass tracts. The “key” is to look for the leads with the negative delta wave, because the negative delta wave “points” to the bypass tract (Figure 8.7). Consider the delta waves in ECG lead I, which is a “left-sided” lead. Delta waves in lead I are negative for left free wall tracts, are biphasic (or isoelectric) for left posterior to right posterior tracts, and are positive for right free wall tracts. The delta waves in lead V1 (a right-sided lead) are positive for left free wall and posterior septal tracts and negative for right free wall tracts. They are biphasic (or isoelectric) for anteroseptal tracts.

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Fig. 8.6 Location of bypass tracts. The anatomic structures shown in this ﬁgure are the mitral valve (MV), the tricuspid valve (TV), the coronary sinus (CS), and the His bundle (H). LFW, left free wall tracts; LPS, left paraseptal tracts; PS, posteroseptal tracts; RPS, right paraseptal tracts; RFW, right free wall tracts; AS, anteroseptal tracts; MS, midseptal tracts; MS(L), leftsided midseptal tracts. See text for details.

Fig. 8.7 Electrocardiographic manifestations of the major categories of bypass tracts. Typical electrocardiographic patterns are shown for left free wall bypass tracts (LFW), right free wall tracts (RFW), posteroseptal tracts (PS), and anteroseptal tracts (AS). See text and Table 8.1 for details.

224 II Electrophysiology Testing for Cardiac Arrhythmias Table 8.1 Electrocardiographic Localization of Bypass Tracts. Location of tract Characteristics of preexcited QRS Left free wall Right free wall Posteroseptal Anteroseptal Midseptal

Negative delta wave in AVL and often in lead I. Positive delta wave in inferior and precordial leads. Normal QRS axis Negative delta wave in leads III and AVF. Positive delta waves in leads I and II. Normal QRS axis Negative delta waves in inferior leads. Positive delta waves in leads I and AVL. R/S ratio in V1 < 1; left superior axis Negative delta wave in leads V1 and V2. Positive delta wave in leads I and II. Normal QRS axis ECG similar to anteroseptal, except that in inferior leads, delta waves are not positive

The delta waves in leads II, III, and AVF (inferior leads) are negative for posterior septal tracts and become positive as the tracts move anteriorly toward the anteroseptal regions. Based on this general concept, and on the more speciﬁc criteria listed in Table 8.1, a very good idea of the location of a bypass tract can be ascertained before the electrophysiologic procedure is begun — and thus, before an accurate preliminary action plan can be made. Considerations for successfully mapping and ablating bypass tracts

Before outlining speciﬁc approaches to various types of bypass tracts, let us review some general considerations for successfully mapping and ablating these tracts. 1 Mapping can be conducted on either the atrial or ventricular aspects of the AV groove. In general, when mapping on the ventricular aspect, antegrade conduction over the bypass tract (i.e., the delta wave) is mapped. Maximal preexcitation is helpful in mapping the delta wave. This can be accomplished by pacing the atrium at a rate that maximizes preexcitation, or by administering drugs (such as verapamil) that increase refractory periods in the normal conducting system. When mapping on the atrial aspect of the AV groove, or when mapping concealed bypass tracts, retrograde conduction over the bypass tract is studied. This is best accomplished during orthodromic macroreentrant tachycardia (i.e., tachycardia that uses the bypass tract for retrograde conduction and the normal conducting system for antegrade conduction), or with ventricular pacing at a rate that optimizes retrograde conduction via the bypass tract.

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2 When the mapping catheter is located near the bypass tract (whether on the atrial or ventricular aspect of the AV groove), the interval between the atrial and ventricular depolarizations (assuming that either antegrade or retrograde conduction of impulses is occurring across the bypass tract) will be short. Generally, the localized AV interval is no greater than 60 msec, and sometimes the atrial and ventricular depolarizations are virtually continuous (Figure 8.8). 3 When the mapping catheter is near the bypass tract and preexcitation is occurring, the local ventricular depolarization should be earlier than the earliest ventricular depolarization seen on any surface ECG lead. 4 Loss of preexcitation (i.e., disappearance of the delta wave) when pressure is applied with the tip of the mapping catheter is an excellent indication that the site of the bypass tract has been localized. 5 In many patients, a localized potential from the bypass tract itself can be recorded (Figure 8.9). These bypass tract potentials tend to be relatively low in amplitude, but tend to have discrete, sharp onsets. They generally resemble His bundle electrograms more than they do the slow pathway potentials seen when mapping the slow AV nodal pathways. Sometimes it can be difﬁcult to differentiate between a bypass tract potential and a part of the atrial or ventricular depolarizations. Pacing techniques can often be used to demonstrate that the bypass tract potentials are distinct from either the atrial or ventricular potentials. Demonstrating a clear-cut bypass tract potential is an excellent indication that RF ablation at that site will be successful.

Fig. 8.8 Depiction of the narrow AV interval seen when the mapping catheter is in proximity to the bypass tract. Compare to the more “usual” AV interval shown in Figure 8.5. When mapping bypass tracts, generally, the optimal localized AV interval is less than 60 msec.

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Fig. 8.9 Recording of a bypass tract potential. Often, a localized potential from the bypass tract itself (AP, “accessory pathway” potential) can be recorded from a wellpositioned mapping catheter.

6 Unipolar recordings from the tip of the mapping catheter can be extremely helpful in localizing the bypass tract, as unipolar recordings give information about the direction of the cardiac impulse being recorded (a positive deﬂection means the impulse is moving toward the unipolar electrode, while a negative deﬂection means it is moving away). When the QRS complex is preexcited, the unipolar ventricular electrogram should be predominantly negative (i.e., a QS complex should be recorded). A negative unipolar ventricular electrogram indicates that the electrical impulse during ventricular depolarization is always moving away from the catheter tip — which is possible only if the catheter tip is located at the site of earliest ventricular activation. A negative ventricular deﬂection on the unipolar electrogram is entirely analogous to a negative delta wave seen on the corresponding surface ECG leads. 7 Finally, once the bypass tract has been carefully mapped and it is time to perform the ablation, catheter stability is critical since RF energy must be continuously applied to the target tissue for a sustained period of time (often 60 seconds or longer). The catheter is considered to be sufﬁciently stable when the ratio of the amplitudes of atrial to ventricular deﬂections on the local intracardiac electrogram varies by less than 10%. The approach to bypass tracts according to location Left free wall bypass tracts

More than 50% of bypass tracts referred for RF ablation have been located in the left free wall. These tracts cross the AV groove along the

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anterolateral, lateral, posterolateral, or posterior aspects of the mitral valve annulus. The coronary sinus also courses along the same portion of the mitral annulus, and thus provides a convenient means of mapping the annulus in patients with left free wall pathways. Standard electrode catheters are placed in the high right atrium, His position, and right ventricular apex. A multipolar electrode catheter is placed into the coronary sinus (often, a 10-lead catheter is used), and multiple bipolar recordings are established along the length of the coronary sinus. After the earliest sites of antegrade and retrograde preexcitation are approximated using the electrodes within the coronary sinus, the mapping and ablation catheter is inserted. There are two general approaches for ablating left free wall pathways — the retrograde approach and the transseptal approach. The retrograde approach is used most commonly and usually yields favorable results. The mapping catheter is inserted through a femoral artery and advanced across the aortic valve into the left ventricle. The catheter tip then is maneuvered into the AV groove beneath the mitral valve leaﬂets, and the bypass tract is localized. The transseptal approach also is very effective in skilled hands. The mapping catheter is inserted through a femoral vein and advanced across the intraatrial septum into the left atrium. In most cases, crossing the intraatrial septum requires that a puncture be made through the septal wall, using a catheter-based tool designed speciﬁcally for that purpose. When the transseptal approach is used, the atrial aspect of the mitral annulus is mapped. With either approach, the multipolar coronary sinus catheter is used as a stable reference for guiding mapping maneuvers. Also with either approach, successful ablation of left free wall bypass tracts can be achieved in more than 95% of cases. Right free wall bypass tracts

Right free wall tracts are seen in approximately 10% of patients with bypass tracts referred for ablation. These tracts are more difﬁcult to map and ablate than left free wall tracts because on the right side a stable catheter position is more difﬁcult to attain, and because there is no anatomic structure analogous to the coronary sinus to aid in mapping. Standard electrode catheters are placed in the high right atrium, His position, right ventricular apex, and coronary sinus. The mapping and ablation catheter is usually inserted via a femoral vein, advanced across the tricuspid valve, and then withdrawn so that the mapping electrodes are positioned along the tricuspid annulus in such a way that both atrial and ventricular deﬂections are recorded. Mapping is often conducted

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using the left anterior oblique (LAO) projection, which allows the tricuspid annulus to be visualized as the face of a clock (Figure 8.10). In this projection, the His bundle is located at approximately 1:00 o’clock, and the os of the coronary sinus at approximately 5:00 o’clock. If the bypass tract proves to be difﬁcult to map, or if catheter stability is a problem, alternative approaches can be tried. Introducing the mapping catheter via the superior instead of the inferior vena cava is sometimes helpful. Long intravascular sheaths can also be used to lend stability to the mapping catheter. In experienced hands, right free wall pathways can be successfully ablated in over 90% of cases. Mahaim bypass tracts

Mahaim bypass tracts, as originally described, supposedly connect the AV node either to the right bundle branch (nodofascicular ﬁbers) or to ventricular muscle (nodoventricular ﬁbers). Recently, it has been determined with careful mapping that Mahaim tracts actually do not arise within the AV node itself, but instead arise within atrial muscle. Thus, these bypass tracts actually form connections between atrial muscle and the right bundle branch (atriofascicular ﬁbers) or ventricular muscle (atrioventricular ﬁbers). The original confusion as to their site of atrial insertion arose from the fact that atriofascicular and atrioventricular tracts display the same

Fig. 8.10 Orientation of tricuspid annulus (TV) in the left anterior oblique (LAO) projection. In the LAO projection, the tricuspid annulus can be visualized as the face of a clock, with the His bundle (H) in the 1:00 position and os of the coronary sinus (CS) in the 5:00 position. MV, Mitral Value annulus.

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sort of decremental conduction usually associated with AV nodal tissue; that is, with atrial pacing, faster pacing rates increase the stimulus to delta wave interval, in distinction to a more typical bypass tract where faster pacing rates decrease the stimulus to delta wave interval. Further, Mahaim bypass tracts tend to respond to adenosine similarly to AV nodal tissue. For practical purposes, therefore, while Mahaim ﬁbers turn out to be anatomically distinct from the AV node, they are electrophysiologically similar to the AV node. Conceptually, Mahaim ﬁbers can be visualized as strands of slow AV nodal ﬁbers (i.e., the ﬁbers that course along the tricuspid annulus within Koch’s triangle) that abnormally veer off, bypassing the AV node, and connecting directly to the right bundle branch or right ventricular myocardium. The electrophysiologic characteristics of atriofascicular tracts are as follows. These tracts tend to display relatively little preexcitation during sinus rhythm but yield left bundle branch block (since they connect to the right bundle branch) with atrial pacing or during tachycardia. As noted, these tracts display decremental conduction and responsiveness to adenosine. Retrograde conduction is absent in atriofascicular ﬁbers. The tachycardias mediated by these tracts, therefore, always use the bypass tract in the antegrade direction (and are thus manifested by a left bundle branch block conﬁguration) and the AV node (or a second bypass tract) in the retrograde direction. During preexcitation, the earliest ventricular activation is seen in the apex of the right ventricle, since it is the right bundle branch that is being preexcited. Atrioventricular Mahaim ﬁbers display the same electrophysiologic characteristics, except that the right ventricular apex is not the site of earliest ventricular activation during preexcitation, since it is the ventricular muscle adjacent to the tricuspid valve that is being preexcited and not the right bundle branch. Mapping and ablation of atriofascicular and atrioventricular ﬁbers is performed in a manner similar to that described for other right-sided bypass tracts; except that antegrade mapping must always be performed, since these tracts do not display retrograde conduction. This generally requires mapping either during tachycardia or at an atrial pacing rate that maximizes preexcitation. Mapping is conducted along the tricuspid annulus between the His bundle and the os of the coronary sinus. Posterior septal (and paraseptal) bypass tracts

Posterior septal and paraseptal bypass tracts account for over 20% of bypass tracts referred for ablation (Figure 8.11). Posterior septal tracts cross the AV groove near the os of the coronary sinus, where the right atrium and left ventricle are in proximity. Thus,

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Fig. 8.11 Insertions for bypass tracts located in the posterior septal region. The anatomic structures shown are the left atrium (LA), right atrium (RA), left ventricle (LV), right ventricle (RV), and coronary sinus (CS). Posterior septal tracts (PS) connect the right atrium with the left ventricle. Right paraseptal tracts (RPS) connect the right atrium with the right ventricle. Left paraseptal tracts (LPS) connect the left atrium with the left ventricle. See text for details.

the atrial insertion of a posterior septal tract is in the right atrium, while the ventricular insertion is in the left ventricle. In contrast, right paraseptal bypass tracts cross the AV groove just to the right of this region and connect the right atrium with the right ventricle. Left paraseptal bypass tracts cross the AV groove just to the left of this region and connect the left atrium with the left ventricle. Because the connections of posterior septal, left paraseptal, and right paraseptal tracts are all different from one another, the response to bundle branch block that occurs during macroreentrant tachycardia can be useful in differentiating among these three types of posterior bypass tracts. Recall that when bundle branch block occurs during macroreentrant tachycardia and the block is on the same side as a bypass tract, the cycle length of tachycardia increases (see Figure 6.11). Accordingly, with left paraseptal bypass tracts, the onset of left bundle branch block will increase the cycle length of the tachycardia; whereas for right paraseptal tracts, only right bundle branch block will increase the cycle length. Finally, with posterior septal tracts (which connect the left ventricle with the right atrium), left bundle branch block will prolong the cycle length but right bundle branch block will not.

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When ablating posterior septal or paraseptal tracts, the mapping catheter is inserted ﬁrst into the right atrium. Mapping is begun anteriorly in Koch’s triangle, along the tricuspid annulus near the bundle of His. Gradually, the mapping progresses posteriorly to the os of the coronary sinus. Then the right posterior paraseptal region is explored (posterior to the os of the coronary sinus along the tricuspid annulus), and ﬁnally mapping is performed within the os of the coronary sinus. Posterior septal tracts are associated with anomalies of the coronary sinus in more than 15% of cases — often, a coronary sinus diverticulum is present, and, if present, the bypass tract is almost invariably located in the neck of the diverticulum. An injection of dye into the coronary sinus may be necessary to visualize the anatomy. Ablating within the coronary sinus or other cardiac veins is feasible in these cases, and is usually successful. This procedure does carry the risk of perforation, which can lead to cardiac tamponade. In addition, it has recently been recognized that when ablating within the coronary sinus (especially if a diverticulum exists or if ablation is necessary in the middle cardiac vein), signiﬁcant chronic lesions can be produced in the posterior descending coronary artery. It is likely that using careful temperature monitoring will reduce the incidence of such complications. If the bypass tract cannot be localized using these maneuvers, mapping of the left posterior paraseptal region may be necessary — this requires insertion of a mapping catheter retrogradely across the aortic valve. Generally, at least one attempt at ablating the “earliest” site on the right side is attempted before moving to the left side. Successful ablation of posterior septal and paraseptal tracts can be achieved in 85–90% of patients. Anteroseptal and midseptal bypass tracts

In the preablation era, anteroseptal and midseptal pathways were lumped together as “anteroseptal bypass tracts”, owing to their similar electrocardiographic manifestations. These tracts are now known to be quite distinct and require different approaches during ablation procedures, so their differentiation is important. Bypass tracts arising in the region anterior and superior to the His bundle are termed anteroseptal tracts. Bypass tracts arising in the area between the His bundle and the os of the coronary sinus (i.e., in the triangle of Koch) are termed midseptal pathways (see Figure 8.6). On the surface ECG, anteroseptal pathways display positive delta waves in leads I, II, III, and AVF; normal QRS axis; biphasic or positive delta waves in lead V1; and positive delta waves in V2–V6 (see Figure 8.7).

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The electrocardiographic manifestations of midseptal pathways are similar to those of anteroseptal pathways with the following exceptions: For midseptal tracts close to the AV node, the delta wave is isoelectric (instead of positive) in leads III and AVF. For midseptal tracts closer to the coronary sinus, the delta wave is predominantly negative in leads III and AVF, and isoelectric in lead V1 (Figure 8.12). The techniques used in ablating anteroseptal and midseptal tracts are similar to those used for any other bypass tract. In either case, reference electrodes are placed in the right atrium, His position, coronary sinus, and right ventricular apex. The mapping and ablation catheter is inserted from the jugular or subclavian vein (for anteroseptal tracts) or from the femoral vein (for either anteroseptal or midseptal tracts). For anteroseptal bypass tracts, mapping can be accomplished from either the atrial orthe ventricular aspect of the tricuspid valve. In general, a careful attempt should be made to record the anteroseptal bypass tract potential itself, and to carefully differentiate it from the His potential (since anteroseptal tracts are often in close proximity to the His bundle).

Fig. 8.12 Electrocardiographic differentiation between anteroseptal and midseptal bypass tracts. Midseptal tracts are more posterior than anteroseptal tracts, and thus they tend to have some of the electrocardiographic manifestations of posterior septal tracts. The more posterior the midseptal tracts, the more negative the delta waves in the inferior ECG leads (i.e., leads II, III, and AVF), See text. AS, anteroseptal; MS a, midseptal tracts located relatively anteriorly; MS p, midseptal tracts located relatively posteriorly.

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To differentiate the bypass tract from the His bundle, mapping during macroreentrant tachycardia is often very helpful, since during tachycardia the bypass tract is being depolarized retrogradely and the His bundle antegradely. Administering adenosine to selectively block AV conduction via the normal conducting system is also helpful in differentiating between the two. The procedure for ablating midseptal pathways is similar to the procedure for performing slow pathway ablation in AV nodal reentrant tachycardia. Mapping is performed on the tricuspid annulus, between the His bundle and the os of the coronary sinus. If ablation cannot be accomplished from the right side, left-sided mapping (along the mitral annulus between the His bundle and the os of the coronary sinus) may be required. For both midseptal and anteroseptal bypass tracts that are in close proximity to the AV node or His bundle, ablation should be conducted while the patient is in macroreentrant tachycardia, so that the integrity of the normal conducting system can be closely monitored. In general, successful ablation of these bypass tracts can be accomplished in more than 90% of patients. The incidence of inadvertent, complete heart block is generally reported as being less than 5–10%, but right bundle branch block has occurred in up to 40% of patients who have ablation of anteroseptal tracts.

Ablation of atrial tachyarrhythmias Ablation of focal atrial tachycardias

Focal atrial tachycardias can be paroxysmal or incessant, and, depending on their frequency, duration, and rate, they can produce symptoms that are anywhere from mild to severe. These arrhythmias can be caused by automatic foci, foci of triggered activity, or microreentrant circuits. Because they are focal, atrial tachycardias can often be mapped and are thus amenable to RF ablation. The site of atrial tachycardia is often associated with particular anatomic structures, most commonly the crista terminalis in the right atrium (see below), the ostia of the pulmonary veins in the left atrium, the os of the coronary sinus, and the tricuspid annulus. Ablating atrial tachycardia requires activation mapping — the earliest atrial deﬂection is sought that precedes the P wave on the surface electrogram. Thus, successful mapping depends on one’s ability to induce atrial tachycardia during the ablation procedure or on the presence of incessant or very frequent tachycardia. Application of RF energy should also be performed during the tachycardia.

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Ablation of atrial ﬂutter

Careful mapping of the atria during atrial ﬂutter has revealed this rhythm to be a macroreentrant arrhythmia that, in most cases, arises in the right atrium. In most patients with atrial ﬂutter, the reentrant pathway is highly stereotypical. As a result of the particular pathway taken by this “typical” atrial ﬂutter, this atrial ﬂutter is an arrhythmia that often can be readily ablated. Figure 8.13 demonstrates the typical reentrant pathway for atrial ﬂutter. This schematic depicts the interior right atrium, demonstrating the important anatomic features that determine the reentrant pathway for atrial ﬂutter. Two key features should be noted. First, it is the crista terminalis (a ridge of tissue running roughly from the superior to the inferior vena cava) which presents the electrical barrier that deﬁnes the reentrant circuit and allows atrial ﬂutter to develop. Second, in typical

Fig. 8.13 Typical reentrant pathway for atrial ﬂutter. The right atrium is depicted, including the inferior vena cava (IVC), the superior vena cava (SVC), the tricuspid annulus (TV), the AV node (AVN), the os of the coronary sinus (CS), and the crista terminalis (CT). The CT is a ridge of tissue roughly connecting the SVC and the IVC. In most patients with atrial ﬂutter, the CT functionally divides the right atrium into two sections. The ﬂutter circuit (indicated by the arrows) must pass through the narrow isthmus between the IVC and the tricuspid annulus. This isthmus thus presents a favorable target for ablation. See text.

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atrial ﬂutter, the ﬂutter wave must pass through a narrow isthmus deﬁned by the inferior vena cava and the tricuspid annulus. It is this latter feature that makes RF ablation a viable option for many patients with atrial ﬂutter. If a linear lesion can be made, extending from the tricuspid annulus to the opening of the inferior vena cava, then electrical blockade of the necessary isthmus can be created (Figure 8.14). To accomplish this feat, the ablation catheter is introduced from the femoral vein and advanced into the right atrium and across the tricuspid valve. The tip of the catheter is rotated so that it is inferior to the os of the coronary sinus and is then pulled back to the tricuspid annulus. RF energy is then applied as the catheter is slowly drawn back from the annulus to the inferior vena cava (moving it a few millimeters every 30 seconds or so). The linear lesion thus created must produce a complete electrical blockade between the inferior vena cava and the tricuspid annulus — even a minute discontinuity in the line of block will permit atrial ﬂutter to continue. Complete electrical blockade is conﬁrmed by pacing the atrium immediately adjacent to the line of block and

Fig. 8.14 Placement of lesion for ablating atrial ﬂutter. The anatomic features shown here are the same as in Figure 8.13. The ablation lesion (the dark line indicated by Ls) is depicted. This lesion transects the isthmus between the IVC and the tricuspid annulus, blocking the pathway necessary for typical atrial ﬂutter. See text.

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conﬁrming that the resultant atrial activation on the opposite side of the line of block is late. This indicates that the wave of depolarization must proceed around the entire right atrium to the opposite side of the line of block. Some forms of atrial ﬂutter are atypical — while they are still macroreentrant in nature, their reentrant circuits follow pathways other than the typical one described in Figure 8.13. Such atypical ﬂutters are most often seen in patients who have had prior cardiac surgery and who have surgical scars in the atrium. In these cases, the scar (instead of the crista terminalis) serves as the line of block around which atrial ﬂutter becomes established. The challenge to the electrophysiologist attempting to ablate these arrhythmias is to deﬁne the pathway of reentry and to determine where to make a linear lesion that will render the pathway inoperative. Successful ablation can be achieved acutely in over 90% of patients who have typical atrial ﬂutter. Approximately 10–20% of these will, however, subsequently develop recurrent atrial ﬂutter during the next one or two years. These recurrences are thought to indicate that the linear block made during the ablation procedure was not quite complete. A second ablation procedure is often successful in these patients. Ablation of atrial ﬁbrillation

Ablating atrial ﬁbrillation has been a major challenge to electrophysiologists for nearly 20 years. While a lot of progress has been made especially over the last decade, it still is a challenge. Two different approaches for ablating atrial ﬁbrillation have been used: Destroying the substrate necessary for the propagation of atrial ﬁbrillation, and destroying the triggers that initiate atrial ﬁbrillation. During the late 1990s, most of the emphasis was placed on the former; since the turn of the millennium, interest has clearly shifted toward the latter. Destroying the substrate for atrial ﬁbrillation

Atrial ﬁbrillation is a reentrant arrhythmia quite unlike the “typical” reentrant arrhythmias we have been talking about so far in this book. Atrial ﬁbrillation is not generated by a ﬁxed, localized, and mappable reentrant circuit. Instead, atrial ﬁbrillation is caused by multiple reentrant wavefronts, moving haphazardly across the surface of the atria like a family of tornadoes — continuously colliding with each other, extinguishing each other, and spinning off new twisters. This conceptualization of atrial ﬁbrillation is referred to as the “atrial wavefront” model.

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Just as tornadoes are frequent on the uninterrupted expanse of the Great Plains but almost unheard of in the choppy terrain of the Rocky Mountains, atrial ﬁbrillation occurs only when the atria present a large surface area of contiguous, electrically active tissue. This is why small animal hearts cannot be made to ﬁbrillate. And this is also why procedures that divide the large, contiguous atrial surface into smaller regions can eliminate atrial ﬁbrillation. The “maze” procedure does just that. In the initial surgical incarnation of the maze procedure, the surgeon produced a pattern of transmural incisions within the atria, creating a series of strategically placed linear scars that resemble a maze. These scars prevent the propagation of the wavefronts responsible for atrial ﬁbrillation — just as a series of mountain ranges discourages the formation of tornadoes. While the original surgical maze procedure was highly invasive and was associated with signiﬁcant morbidity, it did indeed prevent the recurrence of atrial ﬁbrillation. Less invasive surgical maze procedures are now being developed and employed with some success — using RF energy or cryo-lesions instead of transmural incisions, in order to minimize morbidity. In general, however, this approach is limited to patients who are already having open heart surgery for some other purpose such as mitral valve replacement. Still, the ability of the surgical maze to prevent atrial ﬁbrillation has provided strong evidence in favor of the atrial wavefront model for atrial ﬁbrillation; and it has stimulated the effort to develop catheter-based maze procedures, to duplicate the success of the surgical approach. As it turns out, seven discrete linear scars (three in the right atrium and four in the left atrium) can approximate the lesions created in the surgical maze procedure. Efforts to develop a catheter maze procedure that can be performed safely and reliably, have until now met with only limited success. The chief problem has been the difﬁculty in creating effective linear lesions with a catheter. These efforts, however, have clearly proven the potential of such a technique. A substantial proportion of patients who have had catheter maze procedures to date (most of whom had refractory arrhythmias) were indeed rendered free of atrial ﬁbrillation. These procedures, however, have been exceedingly tedious and lengthy, and they have resulted in signiﬁcant morbidity (the chief problem being systemic embolization, as a result of catheters being placed in the left heart for extended periods of time). The catheter maze procedure has by no means been abandoned, but many electrophysiologists who were initially excited about this approach have stopped doing it, awaiting technologies and techniques

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that will allow it to be achieved more quickly, more safely, and more simply. Destroying the triggers of atrial ﬁbrillation

Largely because of the frustration that electrophysiologists have experienced in their attempts at the catheter maze approach, the ablation of atrial ﬁbrillation has shifted in recent years to an entirely different direction, namely, eliminating the ectopic foci that trigger the arrhythmia. The reasoning behind this approach is relatively simple. Atrial ﬁbrillation may be an extremely complex reentrant arrhythmia, but it still is a reentrant arrhythmia — which means it must be initiated by a premature impulse. So, why not eliminate the premature impulses that trigger it? The obvious advantage here is that, if the triggering ectopic foci can be identiﬁed, then the ablation procedure becomes focal instead of general, and ablation of atrial ﬁbrillation becomes much simpler. Initial attempts at attacking the ectopic triggers of atrial ﬁbrillation met with poor results, mainly because it is often quite difﬁcult to identify and map spontaneous atrial ectopic beats during an electrophysiology study (ectopic beats being notoriously random in frequency). Eventually, however, studies were conducted in a selected series of patients who had frequent episodes of atrial ﬁbrillation (so that triggers could be more easily evaluated). To everyone’s surprise, it was learned that over 90% of the episodes of atrial ﬁbrillation in these patients were triggered from ectopic beats originating in the pulmonary veins. Further, when these foci were ablated, most of these patients had no further atrial ﬁbrillation during follow-up. Suddenly, the pulmonary veins became the main focus of the ablation of atrial ﬁbrillation. Subsequent studies have conﬁrmed that a high proportion of patients with paroxysmal atrial ﬁbrillation have ectopic foci in the pulmonary veins (especially the left and right superior pulmonary veins). Interest quickly shifted away from trying to identify, map, and ablate speciﬁc ectopic foci in patients with atrial ﬁbrillation, toward performing empirical ablation in or around the pulmonary veins in these patients. After several years of trial-and-error attempts, it seems now to be well established that achieving complete electrical isolation of the pulmonary veins is much more effective in preventing atrial ﬁbrillation than the selective ablation of speciﬁc ectopic foci. Such complete electrical isolation implies either making four complete, circumferential lesions around the opening of the four pulmonary veins, or creating one circumferential lesion that encompasses all four veins.

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Several techniques have been developed (and are still being developed further) for achieving complete electrical isolation of the pulmonary veins. The most promising of these involve catheters that are designed to generate circumferential lesions, using one of several different energy sources, and guided either by echocardiography or by newer mapping techniques, such as electromagnetic or noncontact mapping (see below). Using the most advanced techniques, in experienced hands, electrical isolation of the four pulmonary veins in selected patients with paroxysmal atrial ﬁbrillation has yielded success rates (i.e., a “cure” of atrial ﬁbrillation) in excess of 80%. A substantial minority of patients, however, end up with a unique form of atrial ﬂutter, localized to the left atrium, following these procedures. Some electrophysiologists have taken to routinely “adding” a linear lesion extending from one of the inferior pulmonary veins to the mitral valve annulus after pulmonary vein isolation, just to prevent such an arrhythmia. Obviously, the odds of success in ablating paroxysmal atrial ﬁbrillation in this way depend on achieving complete pulmonary vein electrical isolation, in patients whose triggers for atrial ﬁbrillation are isolated to the pulmonary veins. In the best of circumstances, the success rate in preventing atrial ﬁbrillation is not likely to greatly exceed 90% using pulmonary vein isolation alone, since between 5 % and 10% of patients with paroxysmal atrial ﬁbrillation have ectopic foci elsewhere in the heart (the superior vena cava is the next most common location). Further, while pulmonary vein isolation seems to work reasonably well in patients with paroxysmal episodes of atrial ﬁbrillation, patients with more persistent forms of atrial ﬁbrillation commonly have multiple ectopic sources in several locations other than the pulmonary veins, and the success rate with pulmonary vein isolation is correspondingly much lower. In other words, this is mainly a procedure for patients with paroxysmal atrial ﬁbrillation. Systemic embolization remains a risk of pulmonary vein isolation, although its incidence appears to be much less than with the catheter maze approach. Pulmonary vein stenosis is a potentially devastating complication of pulmonary vein isolation; its onset can be relatively subtle, and it can be quite difﬁcult to manage. With more advanced techniques for creating circumferential pulmonary vein lesions safely and reliably, pulmonary vein stenosis should become largely avoidable. See Chapter 6 for a discussion of the overall management of atrial ﬁbrillation, including a discussion of when ablation may be a good option.

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Ablation of reentrant ventricular tachycardias Ablation of reentrant ventricular arrhythmias is based on the assumption that these arrhythmias have as their origin a ﬁxed, discretely located, reentrant circuit, and that the arrhythmia can be cured if that circuit can be localized and ablated. Mapping ventricular reentrant circuits

The localization of reentrant circuits within the ventricle can usually be accomplished using one or more of several methods: Seeking areas of early ventricular activation; seeking areas of slow, fractionated conduction; pace-mapping; and entrainment. As noted in Chapter 7, reentrant ventricular tachycardia is generally possible only when areas within the ventricular muscle become damaged, either from a myocardial infarction or from some other disease process that produces ﬁbrosis within the ventricular myocardium. These damaged areas provide the substrate for the multiple pathways and the slow conduction that are necessary to sustain reentry. During reentrant ventricular tachycardia, the earliest portion of the QRS complex is generally assumed to arise from the exit point of the electrical impulse as it leaves the damaged area of slow conduction and begins depolarizing normal ventricular myocardium. By recording localized electrograms during ventricular tachycardia, the earliest site of ventricular activation can be assumed to be near the “exit point” of the reentrant circuit. This technique is called activation mapping, and is the one used most frequently in ablating ventricular tachycardia. Ideally, a localized “presystolic” signal, one that is inscribed before the onset of the surface QRS complex, indicates a critical area of the reentrant circuit itself and can pinpoint an appropriate area for ablation (Figure 8.15). To perform such activation mapping, the arrhythmia to be mapped should display the following characteristics. First, the arrhythmia should be monomorphic ventricular tachycardia. Polymorphic arrhythmias are extremely difﬁcult to localize because complexes of different morphologies probably have various exit points and thus tend to map to different areas. Ventricular ﬁbrillation is impossible to localize because it is not a localized arrhythmia — it is more proper to visualize it, as in atrial ﬁbrillation, as a series of tornadoes moving across the myocardial surface. Second, the tachycardia should be relatively slow, because for tachycardias in excess of 220 beats/min, it is virtually impossible to distinguish the QRS complex from the T wave (see Figure 7.5), so distinguishing the “onset” of the QRS complex becomes impossible. Third, the patient should ideally have only one type of ventricular

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Fig. 8.15 Mapping of ventricular tachycardia. By recording intracardiac electrograms from multiple ventricular positions during sustained ventricular tachycardia, the earliest site of ventricular activation is sought (in this example, in the posteroseptal left ventricle). In most individuals, the earliest site of activation corresponds to the location of the reentrant circuit.

tachycardia, because tachycardias of various morphologies tend to imply multiple reentrant circuits. Fourth, when transcatheter ablation is to be used, the patient should be able to tolerate ventricular tachycardia sufﬁciently to allow mapping to proceed. Fifth, the patient should ideally have a discrete myocardial scar rather than a diffuse cardiomyopathy. In this latter condition, results of transcatheter ablations have been poor.

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Even if all these features are present, activation mapping is not always successful, probably because the basic assumptions that make activation mapping an attractive approach are sometimes incorrect. Activation mapping was originally predicated on the assumption that reentrant circuits are relatively small and discrete. It turns out instead that in many patients, the reentrant circuit is relatively large and diffuse, and very complex both in terms of physical geometry and electrophysiologic inhomogeneity. The ﬁgure-of-eight model shown in Figure 8.16 illustrates such a condition. In this model, the reentrant circuit is the result of a line of unidirectional block that is present in an area of damaged myocardium. The spreading electrical impulse encounters this line of block from above and moves around it (Figure 8.16A). It then enters the damaged area of myocardium from below and slowly conducts back through the damaged area. It exits the damaged area into the normal myocardium, thus completing the ﬁgure-of-eight reentrant circuit (Figure 8.16B). Consider the possibilities when one tries to map and ablate such a circuit. A lesion placed at point A in Figure 8.17A will not abolish reentry, despite the fact that lesion A has been placed at the earliest point of ventricular activation. In Figure 8.17B, lesion B has been placed at a critical location in the circuit, but the impulse has found a second exit point, and reentry continues. Therefore, when the reentrant tachycardia is caused by such a mechanism, activation mapping does not always result in successful ablation of the reentrant circuit, even when early activation can be readily discerned. A second method for mapping reentrant ventricular tachycardia is to seek areas of slow, fractionated conduction. Slow conduction is a prerequisite for reentrant arrhythmias, and a lesion placed in such an area should abolish reentry. Areas of slow conduction are sought by not attempting to position an electrode catheter until a region is identiﬁed that yields low amplitude, fractionated signals. One advantage to this type of mapping is that, because areas of slow conduction are depolarized during sinus rhythm as well as during ventricular tachycardia, mapping can sometimes be conducted during sinus rhythm. One of the major problems with mapping areas of slow conduction is illustrated in Figure 8.18. The ﬁgure-of-eight reentrant impulse enters the area of damaged myocardium at several points, each of which yields electrograms showing low-amplitude, fractionated activity. Yet, because most of these areas do not participate in the reentrant circuit, lesions placed in these areas do not interrupt the circuit, and reentry continues (lesions A through D). Only lesion E abolishes reentry in this ﬁgure.

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Fig. 8.16 The ﬁgure-of-eight model of ventricular tachycardia. Substantial evidence now indicates that reentrant ventricular tachycardia operates according to this mechanism in many patients. This fact probably accounts for the difﬁculty electrophysiologists have had in performing successful transcatheter ablation of ventricular tachycardia. (A) A patch of damaged myocardium that is protected in the antegrade direction by a line of unidirectional block. An electrical impulse encountering this line of block is forced around the periphery of the damaged area. (B) The completed reentrant circuit. The electrical impulse enters the damaged area from the retrograde direction. After conducting slowly through the damaged myocardium, it exits back into normal tissue, thus completing the circuit.

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Fig. 8.17 Why activation mapping may not lead to successful ablation of ventricular tachycardia. In this ﬁgure, activation mapping has successfully identiﬁed the point of “exit” from the area of damaged myocardium, and attempts at transcatheter ablation are performed (in this and the next ﬁgure, ablation lesions are denoted by X). In (A), the lesion that has been created is extremely close to the exit point (lesion A), but yet has not been placed in an area critical to the reentrant circuit. In (B), the precise exit point has been ablated (lesion B). Although this lesion has successfully abolished the original reentrant pathway, a second exit point has now appeared, and ventricular tachycardia (probably with a somewhat different morphology) remains.

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Fig. 8.18 Why mapping areas of slow conduction may not lead to successful ablation of ventricular tachycardia. The circulating wavefront enters the damaged myocardium at several points, creating multiple areas that will show localized slow conduction. However, lesions placed at points A through D ablate areas of “by-stander slow conduction” and do not affect the reentrant circuit. Only lesion E has the potential of ablating the arrhythmia.

A third method of mapping reentrant ventricular tachycardia is pacemapping. With pace-mapping, a 12-lead ECG is recorded while pacing from various locations within the ventricle at approximately the same rate as the patient’s ventricular tachycardia, to seeka location that exactly reproduces the QRS morphology seen during ventricular tachycardia. The assumption is that such sites are near the exit point of the reentrant circuit. Pace-mapping often yields locations different from those obtained during activation mapping. As with activation mapping, however, pace-mapping can yield points such as the one shown in Figure 8.17A — these points may be near the exit point but not in a critical area of the circuit itself. Entrainment mapping is a variation of pace mapping. The idea is to pace from various areas within the ventricle during sustained ventricular tachycardia, at a cycle length slightly shorter than that of the tachycardia. If the pacing catheter is located within the zone of slow conduction, entrainment can often be accomplished. Because conduction within the zone of slow conduction is usually functionally unidirectional (that is, “retrograde” conduction does not occur in this zone), the pacing impulse will tend to exit the slow zone at the same point at which the reentrant impulse exits. The electrophysiologist observes an increase in the rate of the ventricular tachycardia during entrainment — equal to the rate of pacing, indicating that the rhythm is

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now in fact a paced rhythm — but with a QRS morphology that is identical to the morphology of the ventricular tachycardia. When entrainment occurs, the catheter is not only likely to be within the zone of slow conduction, but also at a potentially critical point within that zone, i.e., one that is utilized by the reentrant circuit. In practice, mapping of ventricular reentrant circuits usually requires the use of several of these techniques. Ideally, all four methods will result in localizing the reentrant circuit to the same area. More often, different methods of mapping point the electrophysiologist to different locations. As a result, when transcatheter ablation is attempted, multiple lesions often need to be created to affect the arrhythmia. In patients whose arrhythmias and whose underlying cardiac disease are “ideal” for ablation, ventricular tachycardia can be abolished (or at least rendered less problematic), in up to 75% of patients using radiofrequency ablation. The rate of success falls off dramatically if the arrhythmia is not ideally suited for ablation. The morbidity of radiofrequency ablation of ventricular tachycardia appears to be relatively low, especially when compared to surgical ablation, but few large series have been published, and techniques are evolving so rapidly that published series may not reﬂect the current practice. Unfortunately, many ventricular tachycardias are not ideal for ablation. In addition to lacking the “ideal” characteristics listed above, many reentrant ventricular arrhythmias are located in areas that are largely inaccessible by endocardial mapping. These areas include the midmyocardial and subepicardial regions, and the intraseptal areas (all of which are difﬁcult to localize endocardially, and which may not be affected by endocardial RF applications). During surgical ablation of ventricular tachycardia, the same principles of mapping are used, with the exception of pace-mapping (because the open and distorted ventricle is unlikely to yield morphologies during pacing that reﬂect the clinical arrhythmia). Although precise intraoperative mapping is possible, in practice very large surgical lesions are usually created, mainly because one does not expect to have a second chance to surgically ablate ventricular tachycardia. One thus tends to err on the side of creating overly generous rather than overly fastidious lesions. Surgical “cures” of ventricular tachycardia are seen in up to 80% of carefully selected patients (generally patients with discrete anterior ventricular aneurysms and ideal arrhythmias). The major problem with surgical ablation of ventricular tachycardia is the perioperative mortality (usually reported as being between 5% and 15%) and morbidity.

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Ablation of unusual ventricular tachycardias In Chapter 7, we mentioned several unusual types of ventricular tachycardia that do not ﬁt neatly into the standard classiﬁcations of ventricular arrhythmias. As it turns out, at least three of these unusual ventricular tachycardias are often amenable to RF ablation — right ventricular outﬂow tract tachycardia, idiopathic left ventricular tachycardia, and bundle branch reentrant tachycardia. Right ventricular outﬂow tract tachycardia

Right ventricular outﬂow tract tachycardia, an arrhythmia often seen in young patients with apparently normal hearts, is characterized by its left bundle branch block conﬁguration with a relatively narrow QRS complex (usually less than 140 msec). It often presents as repetitive monomorphic ventricular tachycardia (i.e., as extremely frequent nonsustained ventricular tachycardia). This tachycardia originates in the right ventricular outﬂow area, usually just proximal to the pulmonic valve. The arrhythmia is generally not inducible with programmed pacing but can often be induced with an isoproterenol infusion. If so, activation mapping can be performed. Otherwise, pace-mapping is necessary. Fortunately, because these tachycardias are quite focal in origin, pacing from the site of tachycardia produces a QRS complex that is identical to the clinical arrhythmia. Pace-mapping thus tends to be much more reliable for this arrhythmia than for typical reentrant ventricular tachycardia. Successful ablation of right ventricular outﬂow tract tachycardia can be achieved in over 95% of patients presenting with this arrhythmia. Complications are rare but include perforation of the right ventricle and the production of occlusive lesions in coronary arteries overlying the site of ablation. Both of these complications are related to the fact that the right ventricle is a very thin-walled structure, and both can probably be reduced in frequency by monitoring temperature during RF ablation. Idiopathic left ventricular tachycardia

Idiopathic left ventricular tachycardia, also called left posteroseptal tachycardia, is a verapamil-sensitive arrhythmia originating in the posteroapical aspect of the left ventricular septum, in the region of the left posterior fascicle. The arrhythmia displays a right bundle branch morphology with left axis deviation. It is also seen in patients who have otherwise normal hearts. Ablation is conducted by performing activation mapping in the distal left ventricular septum. At the site of earliest ventricular activation, the

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ventricular deﬂection is preceded (by up to 40 msec) by a distinct “fascicular” potential that resembles a His potential. Successful ablation can be performed in approximately 75–80% of patients with idiopathic left ventricular tachycardia. Bundle branch reentrant tachycardia

Bundle branch reentrant tachycardia, as opposed to the other forms of readily ablatable ventricular tachycardias, does not occur in patients who have otherwise “normal” ventricles. Patients with sustained bundle branch reentry generally have underlying nonischemic dilated cardiomyopathy that is relatively severe, and also have intraventricular conduction defects on their electrocardiograms. The arrhythmia is rapid, usually symptomatic (often presenting with syncope or cardiac arrest), and is most often of left bundle branch morphology. The reentrant circuit uses one bundle branch (usually the right bundle branch) in the antegrade direction and the other bundle branch (usually the left) in the retrograde direction (Figure 8.19). Establishing a sustained bundle branch reentrant tachycardia requires a conduction delay within the bundle branches (and thus requires intrinsic conduction system disease). Thus, bundle branch reentry should be suspected in patients with nonischemic cardiomyopathy and intraventricular conduction delays on their 12-lead ECGs, who present with ventricular tachycardia that has left bundle branch morphology. During the electrophysiology study, each QRS complex of the tachycardia is preceded by a His bundle deﬂection. The HV interval during tachycardia may be the same as, slightly longer than, or slightly shorter than that during sinus rhythm, depending on the site of the recording catheter and the conduction velocity in the right bundle branch during the tachycardia. AV dissociation is usually present during bundle branch reentrant tachycardia. During this tachycardia, the interval between the His deﬂection and the right bundle branch deﬂection is usually shorter than during sinus rhythm. This ﬁnding helps to differentiate bundle branch reentry from supraventricular tachycardias with aberrancy (in which the His-toright-bundle deﬂection is normal or prolonged). Further, any variations in the tachycardia cycle length during bundle branch reentry are preceded by variations in the HH interval, that is, by variations in the interval between His spikes in two successive beats of the tachycardia. This is in contradiction to what one would see in other forms of ventricular tachycardia, in which the retrograde activation of the His bundle occurs passively, following ventricular activation.

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Fig. 8.19 Bundle branch reentry. The His bundle and right and left bundle branches are depicted. Sustained bundle branch reentrant tachycardia requires intrinsic conduction delay in the bundle branches, most often manifested by an intraventricular conduction delay on the ECG. In (A), a premature ventricular impulse blocks retrogradely in the right bundle branch (RB), then conducts up the left bundle branch (LB), but ﬁnds the RB still refractory in the antegrade direction. Bundle branch reentry is thus not established. A more appropriately timed premature impulse (B) might encounter very slow retrograde conduction up the LB, so that antegrade penetration of the RB is now possible. A sustained reentrant arrhythmia using the RB antegradely and the LB retrogradely is now established. The resultant ventricular tachycardia will have an LBBB conﬁguration.

Once bundle branch reentry has been conﬁrmed, ablation of the right bundle branch eliminates the reentrant circuit. Ablating the right bundle branch is accomplished by ﬁrst manipulating the ablation catheter to record the His bundle electrogram, and then slowly advancing the catheter until a distinct right bundle branch deﬂection is seen.

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Successful ablation of the right bundle branch can be achieved in more than 95% of patients with bundle branch reentrant tachycardia. Unfortunately, owing to the signiﬁcant underlying cardiac disease that burdens these patients, their long-term prognosis — from both an arrhythmic and a hemodynamic standpoint — remains relatively poor. Many electrophysiologists often consider implanting deﬁbrillators in these patients, even after “curing” their bundle branch reentry.

Newer methods of mapping As we have seen, endocardial mapping has several limitations. Newer methods of mapping are under development in the attempt to get around these limitations, and some have shown great promise. Epicardial mapping

As detailed previously, in some cases — especially in ventricular tachycardias — reentrant circuits may be subepicardial, rendering the endocardial approach to mapping and ablation difﬁcult if not impossible. Various approaches have been tried for mapping epicardially in such cases. Specialized recording catheters can be used within the coronary sinus system to map epicardially. Further, mapping catheters can be inserted into the pericardial space for epicardial mapping and ablation via a percutaneous subxyphoidal approach. At this time, percutaneous epicardial mapping is done only in a few centers. Electromagnetic mapping (also called electroanatomical mapping)

Many electrophysiology laboratories now are equipped with electromagnetic mapping systems (CARTOtm). With this system, three magnets are placed beneath the patient to create a three-dimensional magnetic ﬁeld, and a specialized catheter is placed within the heart that can “sense” the magnetic ﬁeld and locate itself within that ﬁeld. As the catheter is manipulated within the cardiac chamber, the system generates a three-dimensional image of the local cardiac geometry — and of the dynamic electrical activity. This electrical activity can be displayed as an animated representation, allowing reentrant circuits and ectopic activity to be visualized. Noncontact mapping

Noncontact mapping uses a balloon-tipped catheter with a 64-electrode array on the outside of the balloon. The catheter is placed within the blood pool in the appropriate cardiac chamber (hence the “noncontact” mapping), and a computer uses signals from the 64 electrodes to crunch

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out what engineers lovingly call an inverse solution to LaPlace’s transform — and, voila, an activation map is created. A second, “roving” catheter is then placed and manipulated, and from this a geographical representation of the cardiac chamber is generated. The end result is similar to that achieved with electromagnetic mapping — a threedimensional image of the cardiac chamber with activation patterns displayed. Both electromagnetic and noncontact mapping have been used successfully in the mapping and ablation of bypass tracts, focal atrial tachycardias, ventricular tachycardias, and atrial ﬁbrillation. While still expensive, still complex and of limited availability, systems like these are playing a rapidly expanding role in ablation procedures. It is likely that, as such novel mapping systems evolve, they will revolutionize our ability to ablate difﬁcult arrhythmias.

Complications of RF ablation RF ablation carries the same risks as a standard electrophysiology study (discussed in Chapter 4), plus the added risks related to performing the RF ablation itself. The two most common of these are the risk of creating inadvertent, complete heart block (usually when ablating in proximity to the normal conducting system) and the risk of causing cardiac perforation and tamponade (usually when ablating from the atria, the right ventricle, or within the coronary sinus or other cardiac veins). These complications each occur in less than 1–2% of patients treated with RF ablation. Even rarer complications include the creation of arrhythmogenic foci (uncommon since RF energy tends to create homogeneous lesions); production of mitral or tricuspid regurgitation (when ablating at or near the valvular apparatus); systemic embolization (when mapping and ablating in the left heart); pulmonary vein stenosis (when ablating for atrial ﬁbrillation); and the creation of ﬁxed lesions within the coronary arteries. The creation of ﬁxed coronary artery lesions is apparently due to disruption of the media of the coronary artery when RF energy is applied to an adjacent area. Its true incidence is unknown, but it may be of more than passing concern when ablating within the coronary sinus or the cardiac veins. It has also been reported to occur when ablating in the right ventricular outﬂow area. The coronary artery lesions thus created tend to be silent and are therefore likely to be unrecognized, even though they may produce a signiﬁcant degree of obstruction. It is likely that temperature monitoring during ablation will be helpful in avoiding this

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problem. Its incidence and its long-term signiﬁcance still need to be elucidated. Overall, the risk associated with RF ablation is low. For arrhythmias that are life-threatening or signiﬁcantly symptomatic, and that have a high probability of being successfully treated with RF ablation, this is an extremely attractive option. In the author’s opinion, if a patient has an arrhythmia that is readily amenable to RF ablation, then ablation should be strongly considered whenever daily antiarrhythmic drug therapy would otherwise be required.

CHAPTER 9

Cardiac Resynchronization: Pacing Therapy for Heart Failure

Electrophysiologists have always been intrigued with the notion that, somehow, pacemakers could improve the function of the failing heart. When permanent pacemakers were ﬁrst developed, many thought they could improve cardiac function in patients with heart failure simply by increasing the heart rate. Since cardiac output equals stroke volume times heart rate, they reasoned, pacing the heart a little faster ought to increase cardiac output. What they failed to realize (hemodynamics never being the strong suit of most electrophysiologists) was that the heart does not determine the cardiac output; the body does. The heart merely responds to the metabolic demands of the body. So, unless a patient is in overt low-output failure at rest, increasing the resting heart rate does not appreciably increase cardiac output. Instead, since the heart can only pump whatever volume of blood the body returns to it, the stroke volume falls; the cardiac output remains the same, only now at the cost of an increased heart rate and higher cardiac workload. If anything, patients with heart failure feel worse with pacemaker-induced rapid heart rates. Then, a few years later when dual-chambered pacemakers became available, many electrophysiologists decided to goose the other determinant of cardiac output — the stroke volume — by ﬁguring out how to optimize the AV delay. This goal proved elusive. Attempts at optimizing the AV delay generated a confusion of literature — some experts proposing shorter AV delays, others proposing longer ones — that successfully boosted a few academic careers but not in any reliable way the cardiac function of patients with heart failure. So we can readily understand why, when yet another attempt at improving heart failure with pacing therapy was proposed in the mid1990s, it was initially viewed with great skepticism. This time, however, the pacing therapy worked. 253

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Cardiac resynchronization therapy (CRT) How it works

Cardiac resynchronization therapy (CRT), also referred to as biventricular pacing, is aimed at improving the disordered patterns of ventricular contraction — referred to as ventricular dyssynchrony — seen in some patients with heart failure. CRT is accomplished, in general, by pacing both ventricles simultaneously, thus improving the coordination of dyssynchronous left ventricular contraction. CRT pacemakers have three pacing leads instead of two: A right atrial lead, a right ventricular lead, and a left ventricular lead. They work similarly to DDD pacemakers except for two things. First, with CRT pacing, both ventricles are paced instead of just the right ventricle. Second, biventricular pacing itself, rather than rate support, is the primary desired therapy — CRT pacemakers are thus programmed to pace virtually 100% of the time, under all conditions. CRT pacemakers are used to correct ventricular dyssynchrony. Ventricular dyssynchrony is most obviously present in patients with wide QRS complexes. Since the QRS complex reﬂects the activation sequence of the ventricular muscle, a wide QRS complex indicates that the ventricles are being activated abnormally. Speciﬁcally, a bundle branch block implies that one ventricle is being activated before the other — that is, the ventricles are being activated sequentially instead of simultaneously. This sort of ventricular dyssynchrony does not produce any noticeable hemodynamic consequences in people with otherwise normal hearts. But in patients with systolic dysfunction, ventricular dyssynchrony can produce enough inefﬁciency in ventricular contraction to cause or worsen symptoms of heart failure. In these cases, by pacing both ventricles simultaneously one often can resynchronize ventricular contraction sufﬁciently to improve ventricular efﬁciency, reduce symptoms, and improve clinical outcomes. Figure 9.1 illustrates how left ventricular dyssynchrony caused by left bundle branch block can affect ventricular function in a patient with heart failure. The panel on the left shows a dilated left ventricle at enddiastole. The middle panel shows the ﬁrst 60 msec of systole. Here, the septum (which is activated along with the right ventricle) is already contracting, but the left ventricular free wall has not yet been activated (due to the bundle branch block). In fact, the left free wall bulges outward. The panel on the right shows the last 60 msec of systole. The left ventricular free wall has ﬁnally been activated and is contracting; but now the septum, which has already ﬁnished contracting, is pushed outward. As a result, with each systole, much of the precious energy being expended by

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Figure 9.1 How ventricular dyssynchrony causes reduced ventricular function. The three panels in this ﬁgure illustrate ventricular systole in a patient with cardiomyopathy and left bundle branch block. The panel on the left shows the dilated left ventricle at end-diastole. The middle panel shows the ﬁrst 60 msec of systole. Here, the septum (which is activated along with the right ventricle) is already contracting, but the left ventricular free wall has not yet been activated. In fact, the free wall bulges outward. The panel on the right shows the last 60 msec of systole. The left ventricular free wall is now ﬁnally being activated; but now the septum, which has already ﬁnished contracting, is pushed outward. As a result of this dyssynchrony, with each systole, much of the energy expended by this diseased ventricle is applied toward creating a useless, swaying, “hula”-type movement, instead of being applied toward ejecting blood into the aorta.

Figure 9.2 How biventricular pacing improves ventricular function. The two panels in this ﬁgure illustrate how biventricular pacing improves the function of the dyssynchronous, cardiomyopathic left ventricle illustrated in Fig. 9.1. The panel on the left shows the dilated left ventricle at end-diastole. The panel on the right shows what happens when biventricular pacing is activated. Here, the right and left ventricles are paced simultaneously; both the septum and the left ventricular free wall contract at the same time. The energy expended by the ventricle now goes toward ejecting the blood, instead of merely swishing it around inside the cardiac chamber. Ventricular contraction becomes much more efﬁcient and effective.

this diseased ventricle is used to create a useless, swaying, “hula”-type movement, swishing blood around inside the cardiac chamber instead of ejecting it out into the aorta. Figure 9.2 illustrates how CRT might beneﬁt such a ventricle. The panel on the left again shows the same dilated left ventricle at end-

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diastole. The panel on the right shows what happens when biventricular pacing is activated. Here, the right and left ventricles are paced simultaneously; both the septum and the left ventricular free wall contract at the same time. The energy expended by the ventricle now moves toward ejecting blood. Ventricular contraction becomes much more efﬁcient and effective. Between 20% and 30% of patients with congestive heart failure have intraventricular conduction delays, and in most of these, it is left ventricular activation that is delayed. The effects of CRT

Several clinical studies have documented the beneﬁts of CRT in appropriately selected patients. Hemodynamic effects

CRT has consistently yielded improved hemodynamic function in patients with heart failure and left bundle branch block, including improved cardiac output and cardiac index, increased aortic pulse pressure, and reduced pulmonary capillary wedge pressure. Contractility

Measures of left ventricular contractility improve with CRT, including enhanced global contraction and increased left ventricular ejection fractions. In contrast to other forms of therapy that have boosted ventricular contractility in patients with heart failure (such as the inotropic agents amrinone and milrinone), CRT actually reduces myocardial energy expenditures. Thus, ventricular contraction is not only more effective but also more efﬁcient. Reverse remodeling

Remodeling of the left ventricle — manifested by ventricular dilation, increased ventricular mass, and reduced ejection fraction — is a fundamental response to reduced systolic function. In essence, the cardiac enlargement that occurs with remodeling is a compensatory mechanism that allows the ventricle to eject a near-normal stroke volume despite reduced contractility. Aside from the fact that remodeling itself is ultimately harmful, the degree of remodeling reﬂects the degree of systolic dysfunction. CRT has been demonstrated to reverse left ventricular remodeling. Speciﬁcally, it has been shown to reduce the end-systolic and enddiastolic dimensions of the left ventricle, as well as reducing the left

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ventricular mass. This reverse remodeling is thought to reﬂect a fundamental improvement in ventricular systolic function. Clinical studies with CRT

Several randomized clinical trials have now been completed, testing the effect of CRT in patients with heart failure due to systolic dysfunction. In general, these trials have enrolled patients with NYHA Class II–VI heart failure, QRS prolongation (at least 120–140 msec), and left ventricular ejection fractions of 0.35 or less. The major clinical trials with CRT are summarized in Table 9.1. From these trials — and from meta-analyses using these and other trials — CRT has been convincingly shown to accomplish the following in appropriately selected patients: • reduced mortality from progressive heart failure • reduced hospitalizations from heart failure • improved ejection fraction • improved quality of life and functional class Furthermore, the addition of ICD therapy to CRT has been shown to signiﬁcantly improve the mortality beneﬁt seen with CRT alone. Indications for CRT

Currently, the joint American College of Cardiology/American Heart Association/Heart Rhythm Society statement on pacing in heart failure indicates CRT therapy for patients with refractory NYHA Class III or IV heart failure; with either idiopathic dilated or ischemic cardiomyopathy; with a QRS interval of 130 msec or greater; with LV end-diastolic diameter of greater than or equal to 55 mm; and with a left ventricular ejection fraction of less than or equal to 0.35. CRT is currently listed as Class IIA indication; i.e., the weight of evidence is in favor of the usefulness of this therapy, but there is a divergence of opinion. This current joint statement does, however, not take into account either the COMPANION trial or the CARE-HF trial; the two most recent (and largest) clinical trials, both showing signiﬁcant survival beneﬁts with CRT (see Table 9.1). It is very likely that with the next release of this joint statement on pacing and heart failure, CRT will be given a Class I indication, indicating that there is general agreement the therapy is useful and effective. It ought to be noted further that the vast majority of patients with an indication for CRT therapy also have an indication for an implantable deﬁbrillator (see Chapter 7); so the great majority of patients with heart failure who are candidates for CRT should receive CRT devices that also provide ICD therapy (referred to as CRT-D devices).

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Table 9.1 Major Randomized Trials With CRT. This table summarizes the major randomized clinical trials testing CRT in patients who have signiﬁcant heart failure due to systolic dysfunction and wide QRS complexes. These trials conﬁrmed the effectiveness of CRT in improving functional capacity, quality of life, need for hospitalization, and survival. From the COMPANION trial, the addition of an ICD to CRT therapy greatly improves on the survival beneﬁt seen with CRT alone. TStudy

Patient Population

Randomization

Results with CRT

MIRACLE

435 pts, NYHA III, LVEF ≤ 0.35, QRS ≥ 130

BiV vs. no BiV

MIRACLE 2 ICD

369 pts, same as for MIRACLE, but with indication for ICD 48 pts, NYHA III, QRS ≥ 150, no pacing indication

BiV + ICD vs. ICD alone

Improved 6 minute walk, NYHA Class, LVEF, & reduced hospitalization Improved QOL, NYHA Class, peak O2 consumption, & exercise duration Improved 6 min walk, QOL, peak O2 consumption, decreased hospitalization. 85% of patients preferred BiV mode BiV vs. OPT: Signiﬁcant 20% reduction in all cause mortality or all cause hospitalization; non-signiﬁcant 24% reduction in mortality. BiV + ICD vs. OPT: Signiﬁcant 30% reduction in all cause mortality or all cause hospitalization; signiﬁcant 36% reduction in all cause mortality Signiﬁcant reduction in death or hospitalization due to cardiovascular event (primary endpoint). Signiﬁcant reduction in death from any cause (secondary endpoint)

1

MUSTIC

3

COMPANION

CARE-HF

5

4

BiV vs no BiV for 3 months, then cross over for 3 months

1520 pts, NYHA III–IV, LVEF ≤ 0.35, QRS ≥ 120, recent hospitalization for CHF

OPT vs. BiV, and BiV + ICD (1 : 2 : 2)

813 pts, NYHA III–IV, QRS ≥ 120

BiV vs. no BiV

BiV, biventricular pacing; BiV + ICD, CRT device that also has the functionality of an implantable deﬁbrillator; LVEF, left ventricular ejection fraction; NYHA, New York Heart Association functional class; OPT, optimized pharmacological therapy; pts, patients; QOL, quality of life. 1, Abraham WT, et al. N Engl J Med 2002; 346:1845 2, Young JB, et al. JAMA 2003; 289:2685 3, Linde C, et al. J Am Coll Cardiol 2002; 40:111 4, Bristow MR, et al. N Engl J Med 2004; 350:2140 5, Cleland JGF, et al. N Engl J Med 2005; 352:1539

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Implanting CRT devices

The only signiﬁcant difference between implanting a CRT device and a pacemaker (or between implanting a CRT-D device and an ICD) is the need to place an additional lead for left ventricular pacing. In the early days of CRT, left ventricular pacing was accomplished either with epicardial leads (requiring a limited thoracotomy) or with standard transvenous pacing leads — leads not designed for this purpose — placed into the coronary sinus. Left ventricular lead placement, in those days, was a lengthy, tedious, difﬁcult, and often risky procedure. Nowadays, a variety of tools have been developed speciﬁcally for placement of specially designed pacing leads in the coronary venous system. These tools allow the electrophysiologist to rapidly and safely insert left ventricular pacing leads via the coronary sinus. In most cases, these leads can be placed, positioned, and tested within 30 minutes or less. In placing left-sided leads, the os of the coronary sinus is generally ﬁrst engaged with an introducer designed speciﬁcally for that purpose. Dye is injected to visualize the cardiac venous system. A “target” vein is identiﬁed. (Most patients seem to do best with CRT when the left-sided lead is placed in the mid-lateral left ventricle, so the operator looks for a vein that reaches that area.) A pacing lead is chosen whose handling characteristics are likely to suit the anatomy of the target vein, and is then inserted and positioned. In testing the left-sided lead, the operator looks not only for adequate R wave voltage, pacing threshold, and impedance measurements, but also for evidence of diaphragmatic stimulation — the most common problem with pacing from the coronary veins. If diaphragmatic stimulation is seen, the lead needs to be repositioned. Coronary sinus leads are now available that can be “electronically repositioned” by changing the vector conﬁgurations of available electrodes. Diaphragmatic stimulation can usually be circumvented in this way without having to physically reposition the lead. Coronary sinus perforation and subsequent pericardial tamponade is the main complication (aside from diaphragmatic stimulation) unique to left-sided lead placement. This complication is rare with today’s implantation tools. Adequate placement of a left ventricular lead can be accomplished today via the coronary sinus approach in well over 90% of patients. Occasionally however, pacing the left ventricle still requires an epicardial lead. Tools are being developed to make epicardial lead placement much less invasive and more reliable than it is today; it is likely that within several years, placing epicardial leads will be conducted routinely in the electrophysiology laboratory.

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Unresolved issues with CRT Responders versus non-responders

The results reported from the randomized trials referenced in Table 9.1 are based on population statistics — that is, these trials measure the average response to CRT in a population of patients. And on average, the population does quite well. There is, however, a unique feature of CRT that virtually compels physicians to judge its beneﬁt on an individual basis rather than on the basis of population statistics; namely, in many patients receiving CRT, the response is quite dramatic. Patients often improve rapidly from NYHA Class III to I, or from Class IV to II, and are able to accomplish physical tasks they have not been able to perform for months or years. These patients are exceedingly grateful for their new lease on life, and accordingly, the doctor is exceedingly gratiﬁed. This is amazing stuff. Indeed, it is so wonderful that it has become a virtual expectation, and when patients do not experience a dramatic improvement, they are labeled “non-responders”. It is estimated that roughly between 40–60% of patients who are receiving CRT have a fairly dramatic response; accordingly, the remainder are usually considered to be non-responders. The widespread notion that there are responders and non-responders to CRT, while probably true, can have inappropriate consequences if we are not careful. On one hand, this notion is stimulating device manufacturers and researchers to look for ways to optimize CRT (more on this below) in an effort to convert more non-responders to responders. This effort is likely to yield signiﬁcant beneﬁts, and to result in substantial improvements in the technology and the art of CRT. But on the other hand, this notion is also leading payers to question why they should buy CRT devices for 100 patients when only 50 or so are going to beneﬁt from the device. Their efforts lean less toward optimizing CRT and more toward ﬁguring out how to identify and withhold this therapy from likely non-responders. (We see thus once again a familiar pattern — after insisting on and receiving randomized clinical trials to prove a population beneﬁt for a therapy that often provides obvious and dramatic individual beneﬁts, payers then try to ignore the population beneﬁts deﬁned by those trials, and instead seek to identify individuals on whom not to spend money.) All this means is that we have to be very careful about how we deﬁne “non-responders”. The way in which this term is commonly used today, a non-responder is a patient who has not experienced drama. But this view is shortsighted and, probably, wrong. It seems unlikely, for instance,

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that CRT would produce an “all-or-nothing” effect, where either patients would have remarkable, raising-the-dead-style symptomatic improvement, or no improvement at all. More likely, some patients are beneﬁted by CRT in a more subtle way — such that, for instance, they may not feel dramatically better, but the “trajectory” of their illness has changed so that they have fewer hospitalizations over a given period of time, or their risk of dying is reduced. As it turns out, these more subtle beneﬁts are the very beneﬁts that the randomized trials were designed to measure. From these trials, the magnitude of overall beneﬁt to the population probably cannot be explained by the 40–60% of patients who (if the “responder/non-responder” parameter had been tabulated) would have been classiﬁed as dramatic responders. For instance, in the CARE-HF study, mortality in the CRT group was reduced by 33%, a magnitude that would be very difﬁcult to attribute to the 50% or so who may have responded “dramatically” to the therapy. More likely, this impressive beneﬁt in CARE-HF was distributed among both “dramatic responders” and “non-dramatic responders”. And ﬁnally, evidence is accumulating that even more subtle measures of CRT efﬁcacy — such as reverse remodeling — may continue to improve for at least 12 months after CRT is initiated, even in so-called “nonresponders”. This reverse remodeling suggests that some fundamental improvements in ventricular systolic function are occurring over time — and may be present whether or not a dramatic reduction in symptoms has been seen. By insisting on a dramatic response as the sole recognized beneﬁt of CRT, we are creating unreasonable expectations on the part of our patients, the payers, and ourselves. If we must identify certain individuals as non-responders, we at least ought to be circumspect about how we do so. We should deﬁne “non-responder” in a way that allows for the more subtle — but still substantial — beneﬁts of CRT. Doing so would improve our chances of actually ﬁguring out how to maximize the beneﬁts of CRT, and it would also reduce the temptation we otherwise create for payers to withhold CRT from anyone who doesn’t seem likely to turn cartwheels within 48 hours of implantation. Optimization of CRT

Beyond the original notion that pacing the ventricles simultaneously would help to resynchronize dyssynchronous ventricular contraction, relatively little has been accomplished so far in systematically studying how the beneﬁts of CRT might be optimized in each individual patient. Several methods for optimizing CRT have been proposed; and, if

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developed sufﬁciently, one or more of these may improve the overall beneﬁts of CRT. AV interval Despite the spotted history (described earlier) of AV interval optimization in improving the hemodynamics of failing hearts, there is reason to believe that AV optimization may be an important factor in CRT. Speciﬁcally, the chief concern is with the left atrial to left ventricular (LA-LV) interval. Since pacemakers — even CRT pacemakers — sense only the right (and not the left) atrial electrogram, any intra-atrial conduction delay (i.e., a conduction delay from the right to left atrium) is not taken into account. In other words, the “A” in AV interval is the right atrium — the left atrium is ignored. Therefore, in the setting of an intraatrial conduction delay, during CRT the programmed AV delay may result in an effective LA-LV interval that is “too short”. That is, left ventricular pacing may occur before left atrial contraction is completed, and as a result, left ventricular stroke volume may be systematically reduced during CRT. Whether this is more than a theoretical problem, and whether optimization of LA-LV intervals would improve the effects of CRT in some or all patients, has not been sufﬁciently studied. It is certainly one area of concern in the optimization of CRT. V-V interval Classically, CRT is accomplished by pacing the left ventricle simultaneously with right ventricular activation (or pacing). It may, however, be the case that different timing sequences between the two ventricles (the V-V interval) would improve the efﬁcacy of CRT in some patients. Data exists, for instance, suggesting that in some patients, pacing the left ventricle only (that is, in advance of any right ventricular activation) may be better than biventricular pacing. The V-V interval ought to be viewed as a continuum of potential ventricular activation sequences, all the way from right-ventricular-only pacing (i.e., the pacing mode used in all “standard” pacemakers) to leftventricular-only pacing. For all we know, the optimal V-V interval may vary from patient to patient. CRT devices exist today that allow the physician to vary the V-V interval — but this feature is marketed with few instructions. The clinician has no objective guidance in how to choose the most appropriate V-V interval. Systematic studies are needed to assess whether varying the

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V-V intervals makes a substantial difference; and, if so, how exactly to optimize this parameter in individual patients. Lead placement and lead number When one stops to think about it, it begins to seem remarkable that we have seen such impressive results with CRT by positioning the left ventricular pacing leads “empirically”, often in whichever location is most readily achievable. Could the results of CRT be improved by objectively assessing which speciﬁc region within the left ventricle ought to be paced in each individual, and then taking pains to position the lead in the optimal spot? Some evidence exists (from MRI studies) suggesting that this may be so. Speciﬁcally, there may exist in dyssynchronous left ventricles a “sweet spot”, such that placing the pacing electrode in that spot yields much better resynchronization than placing it just a few centimeters away. Perhaps some patients have more than one “sweet spot”, and perhaps two or more left ventricular electrodes would need to be positioned, quite precisely, in order to truly optimize CRT. Optimal lead placement — and the optimal number of leads to use — is another area in great need of systematic investigation. Measuring dyssynchrony The methodology we currently use to detect left ventricular dyssynchrony — i.e., looking for the presence or absence of an intraventricular conduction delay — is neither particularly sensitive nor speciﬁc. Substantial ventricular dyssynchrony can exist in the absence of an obvious conduction delay, and some patients with conduction delays may not have much dyssynchrony at all. If CRT truly works by resynchronizing the contraction of a dyssynchronous left ventricle, then it seems obvious that to really optimize CRT we need to have an objective, reproducible way to measure dyssynchrony, both before and during CRT pacing. Unfortunately, we do not. Cardiac MRI shows much promise in this area but is not readily available — and it is problematic to perform MRI scans in patients with CRT devices. Tissue Doppler echocardiography (TDE) is also promising, but remains poorly standardized, and its results sometimes appear to be quite operator-dependent. While current methods fall short of the goal, the clinical need for a method of reproducibly measuring ventricular dyssynchrony has now been widely recognized. A lot of work currently aims at accomplishing this, and it is probably only a matter of time before this need is met. When that happens we can expect improved tools for fully optimizing CRT to follow rapidly.

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Should CRT be the standard mode of pacing?

If spontaneous left bundle branch block produces ventricular dyssynchrony, and is thus detrimental to patients with systolic heart failure, then wouldn’t iatrogenic left bundle branch block created by right ventricular pacing also be detrimental to these patients? Is it really a good idea for patients who require pacing most or all of the time to have LBBBinducing right ventricular pacing — especially patients with systolic dysfunction? At least two trials suggest that chronic right ventricular pacing is detrimental. In the DAVID trial (Wilkoff BL et al., JAMA 2002; 288:3115), patients who needed ICDs and who also had depressed left ventricular function, were randomized to DDDR pacing with a lower rate limit of 70 beats/min (in order to increase the use of dual chambered pacing), or to VVI pacing at a lower rate of 40 beats/min (to decrease the use of any pacing at all). The hypothesis of this study — which was initiated before CRT, and its implications regarding ventricular dyssynchrony, were widely known — was that chronic A-V pacing would be beneﬁcial in these patients. Instead, the investigators discovered the opposite. Patients randomized to frequent DDDR pacing had a signiﬁcantly higher incidence of death or hospitalization for heart failure than patients randomized to minimal pacing. Most observers attribute these negative results to the dyssynchrony produced by almost constantly pacing the right ventricle in patients with underlying left ventricular dysfunction. Similarly, the MOST trial (Sweeney MO et al., Circulation 2003; 107:2932), examined clinical outcomes, using various pacing modes, in patients with sinus nodal dysfunction. In this trial, patients with higher cumulative percentages of right ventricular pacing also had more hospitalizations for heart failure. These studies clearly do not constitute unassailable proof that chronic right ventricular pacing is detrimental; but, combined with what we’ve learned over the past few years about the beneﬁts of synchronized ventricular contraction, at the very least they add strongly suggestive evidence to that notion. Some experts have already asserted that patients who require constant pacing, and who also have left ventricular systolic dysfunction, should probably be considered for CRT pacemakers. Indeed, the major brake on the more routine use of CRT pacemakers is probably not so much the need to accumulate more clinical data, but the time and effort required to implant a left ventricular lead. So, while nobody is saying yet that biventricular pacing should be the standard

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method of pacing in everybody, we can expect the use of CRT pacemakers to grow signiﬁcantly over the next years; and the rate of this growth is likely to be determined by how rapidly manufacturers can improve the tools for placing left-sided leads.

C H A P T E R 10

The Evaluation of Syncope

The evaluation of patients with syncope (sudden transient loss of consciousness) has classically been difﬁcult. This difﬁculty stems from the very nature of syncope itself: Syncope occurs most often in a sporadic and relatively unpredictable fashion, and between episodes, patients with syncope often appear to be (and frequently are) quite normal. For two reasons, electrophysiologists are now regularly involved in the evaluation of patients with syncope. First, cardiac arrhythmias are often either a direct cause or a prominent feature of syncope. Second, techniques developed in the electrophysiology laboratory often have proven helpful in revealing the etiology of syncope. In this chapter, we review the causes of syncope and discuss the evaluation of syncope in light of the lessons that have been learned in the electrophysiology laboratory over the past two or three decades.

Causes of syncope Table 10.1 lists the major causes of syncope, divided into ﬁve major categories. Diagnosing syncope associated with the ﬁrst four categories depends on taking a careful history and performing a careful physical examination. The majority of patients with syncope, however, fall into the ﬁfth category — syncope associated with cardiac arrhythmias. In most cases, therefore, the clinician is left with having to assess whether patients have syncope directly caused by cardiac arrhythmias (bradyarrhythmias or tachyarrhythmias), or whether they have a variant of vasodepressor syncope, in which bradycardia is often a prominent feature of syncope. Bradyarrhythmias that cause syncope

Although bradyarrhythmias have been claimed as a common cause of 266

10 The Evaluation of Syncope 267 Table 10.1 Major Causes of Syncope. Syncope from neurologic disorders Vertebrobasilar transient ischemic attacks Subclavian steal syndrome Syncope from metabolic disorders Hypoxia Hypoglycemia

Normal pressure hydrocephalus Seizure disorders Hyperventilation

Syncope from psychiatric disorders Panic disorders

Hysteria

Syncope from mechanical cardiac disease Aortic stenosis Mitral stenosis Pulmonary stenosis Global ischemia Aortic dissection

Obstructive cardiomyopathy Left atrial myxoma Prosthetic valve dysfunction Pulmonary embolus Pulmonary hypertension

Syncope associated with cardiac arrhythmias Bradyarrhythmias — sinus node dysfunction, AV conduction disease Tachyarrhythmias — supraventricular and ventricular tachyarrhythmias Vasodepressor syncope

syncope, they actually cause less than 5% of syncopal episodes. Nonetheless, bradyarrhythmias must be regarded as an important cause of syncope because they are always completely treatable. The evaluation of patients with bradyarrhythmias has been discussed in detail in Chapter 5. In this section, we review the causes and evaluation of bradyarrhythmias only brieﬂy. Sinus nodal dysfunction

Abnormalities of the sinus node are common in elderly patients and are most often due to idiopathic ﬁbrous degeneration of the sinus node. Sinus nodal dysfunction is frequently associated with a similar ﬁbrous degeneration of the AV conduction system, producing AV block, or of the atrial tissue, producing atrial tachyarrhythmias. Although sinus nodal disease is most often benign, the potential for sudden death is real in patients whose sinus nodal dysfunction is severe enough to produce syncope. In most patients with syncope due to sinus nodal dysfunction, abnormalities of the sinus node are overt, and are usually seen during simple cardiac monitoring. Occasionally, however, electrophysiologic testing is needed to diagnose sinus nodal dysfunction even in these patients. Therefore, electrophysiologic testing should be considered in patients

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with syncope when the etiology remains unknown after a full evaluation, especially in elderly patients. AV block

On one hand, AV nodal disease is a rare cause of syncope. On the other hand, block in the His-Purkinje tissue is the most common cause of syncope due to bradyarrhythmias. When syncope is due to AV block, the ECG and cardiac monitoring most often reveal clues as to the etiology of syncope. Obviously, complete heart block in a patient presenting with syncope is an indication for pacing. Second-degree AV block should also be regarded as a strong clue. Even more subtle ﬁndings that can usually be safely ignored, such as intraventricular conduction disturbances or ﬁrst-degree AV block, should be regarded with a high degree of suspicion in patients presenting with syncope. In such patients, electrophysiologic testing should be strongly considered, especially if no other etiology for syncope presents itself. Tachyarrhythmias that cause syncope Supraventricular tachycardias

Although supraventricular tachycardias are relatively frequent arrhythmias, they only rarely cause syncope. In most cases in which syncope is associated with supraventricular tachycardia, a second condition is responsible for the syncope. Most commonly, this second condition is sinus nodal dysfunction. In a patient with sinus nodal dysfunction, supraventricular tachycardia (usually atrial ﬁbrillation or ﬂutter) causes exaggerated overdrive suppression of the diseased sinus node. When the arrhythmia terminates, there is a prolonged sinus pause leading to loss of consciousness. Less commonly, syncope can accompany supraventricular tachycardias that occur without concomitant sinus nodal dysfunction. In these cases, recent evidence suggests that syncope is the result of a vasodepressor reﬂex, and that the tachycardia itself may simply be the triggering stimulus for the vasodepressor response that produces syncope. When syncope is associated with supraventricular tachycardia, loss of consciousness is almost always preceded by a prominent and unambiguous sensation of palpitations. Such a history should lead the physician immediately to suspect tachycardia as an etiology. Electrophysiologic testing should be considered early in the evaluation of such patients. Ventricular tachyarrhythmias

Although ventricular arrhythmias were not generally recognized until the mid-1980s as a major cause of syncope, it is now apparent that these

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arrhythmias are frequently responsible for syncope, especially in patients with underlying cardiac disease. Ventricular tachycardia or ﬁbrillation probably represents the cause of syncope in up to 40% of patients with heart disease who present with this symptom. Because syncope due to ventricular tachyarrhythmias is a sign of impending sudden death, the new onset of syncope in patients with signiﬁcant underlying heart disease should be treated as a medical emergency. Syncope caused by ventricular tachyarrhythmias usually occurs suddenly and without warning, although in some patients with sustained ventricular tachycardia, the sensation of a rapid heart rate may precede loss of consciousness. The syncope can be quite ﬂeeting, lasting only for moments, or it may present as dramatically as a self-terminating cardiac arrest. No other cause of syncope is likely to produce the type of pulseless, apneic, cyanotic patient produced by a ventricular arrhythmia. Many patients referred to electrophysiologists for syncope of unknown etiology are reclassiﬁed as having had an aborted cardiac arrest after careful interrogation of witnesses. Because most ventricular tachyarrhythmias are reentrant in nature, and because most reentrant circuits require the substrate produced by myocardial ﬁbrosis, ventricular arrhythmias are unlikely to be the cause of syncope unless a disorder of the ventricular myocardium is present. When such myocardial disease is present, however, ventricular arrhythmias must be considered as being the most likely cause of syncope until proven otherwise. When evaluating a patient with syncope of unknown etiology, one of the ﬁrst questions the physician must answer is whether the patient has underlying cardiac disease. If so, then the physician’s focus must immediately shift away from merely preventing syncope and toward preventing sudden death. Accordingly, if a careful history and physical examination do not yield the cause of syncope, a noninvasive cardiac workup to assess the status of the ventricular myocardium must be considered an essential part of the evaluation of the patient with syncope. If ventricular function is normal, ventricular arrhythmias can usually be dismissed as a cause for syncope. On the other hand, if there are segmental wall motion abnormalities or if the left ventricular ejection fraction is reduced, potentially lethal ventricular arrhythmias must be strongly considered. The signal-averaged ECG may also help to determine the likelihood that ventricular arrhythmias are the cause of a patient’s syncope. The sensitivity of the signal-averaged ECG has generally been reported as being 73–89%, and the speciﬁcity from 89% to 100%, in predicting whether a patient presenting with syncope will have a positive electrophysiologic study.

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Ambulatory monitoring should play a very small role in diagnosing ventricular arrhythmias as a cause of syncope for three reasons. First, ventricular arrhythmias producing syncope are sporadic and unpredictable. The odds of capturing a syncope-producing ventricular arrhythmia while monitoring for a few days or a few weeks are small; and in a patient with underlying cardiac disease, the absence of such arrhythmias on ambulatory monitoring is meaningless. Second, the presence or absence of asymptomatic ventricular ectopy in such patients has extremely small speciﬁcity (so ﬁnding ectopy on ambulatory monitoring does not bring the clinician any closer to making a diagnosis). Third, once a patient with signiﬁcant underlying heart disease has syncope of unclear origin, that patient must be presumed to be in imminent danger of sudden death, and the time for leisurely outpatient monitoring has passed. That patient should be evaluated as if he or she had suffered not “just” syncope, but an aborted cardiac arrest. Once it has been determined that ventricular arrhythmias are reasonably likely to be the cause of a patient’s syncope, that patient should immediately be admitted to a monitored bed until lethal ventricular tachyarrhythmias either have been deﬁnitively ruled out or adequately treated. In such patients, the electrophysiology study is often the most direct way of determining the cause of syncope and deciding on appropriate therapy. Vasodepressor syncope

Vasodepressor syncope is by far the most common cause of syncope. The fact that vasodepressor syncope is known by so many names (including vasovagal syncope, cardioneurogenic syncope, and reﬂex syncope) is a reﬂection of the fact that its mechanism is poorly understood. To make matters worse, clinical syndromes that are almost certainly subcategories of vasodepressor syncope (Table 10.2) have most often been discussed in the literature as if they were completely unique and unrelated entities. This practice has led clinicians to the widespread misconception that there must be scores of causes of syncope, and accordingly, to a widespread attitude of hopelessness when faced with a patient who has syncope. In fact, patients who are prone to vasodepressor syncope often have a history of multiple syncopal episodes, and their episodes frequently fall into several of the syndromes listed in Table 10.2. Recognition that these different syndromes are merely variants of the same basic mechanism leads the physician immediately to the diagnosis in the majority of cases, and is a major step toward prescribing effective treatment.

10 The Evaluation of Syncope 271 Table 10.2 Syndromes of Vasodepressor Syncope. Presumed afferent pathways

Syndromes

Gastrointestinal/ genitourinary mechanoreceptors

Micturition Defecation

Postprandial Peptic ulcer

Cerebral cortex

Panic or fright Pain

Noxious stimuli

Cranial nerves

Glossopharyngeal neuralgia

Oculovagal

Cardiopulmonary baroreceptors

Carotid sinus

Tussive

Cardiac C ﬁbers

Valsalva Upright tilt Jacuzzi Weight-lifting Trumpet playing

Postexercise Volume depletion Pacemaker syndrome Supraventricular tachycardia

The common denominator in all varieties of vasodepressor syncope is most likely the stimulation of the medullary vasodepressor region of the brain stem. The pathways that stimulate the vasodepressor region (afferent pathways) can arise from numerous locations — the resultant clinical syndrome has most often been named by the event that results in afferent stimulation of the medullary vasodepressor region, see Table 10.2. Once the vasodepressor region has been stimulated, that region generates efferent signals that cause both increased vagal tone (via the vagus nerve) and vasodilation (by pathways that are not well understood). Diminished cardiac ﬁlling and bradycardia follow, leading to syncope. It should be recognized that although bradycardia is therefore often a prominent feature of this type of syncope, it is only rarely as important as vasodilation in producing symptoms. This is why therapy with pacemakers is usually not of signiﬁcant beneﬁt to patients suffering from vasodepressor syncope. This is also why the author has chosen to use the term “vasodepressor syncope” from the available menagerie of names. In many of the syndromes listed in Table 10.2, stimulation of the cardiac C ﬁbers (mechanocardiac receptors in the left ventricle) appears to be the origin of afferent stimulation of the vasodepressor region. The C ﬁbers are stimulated when a volume-depleted ventricle is contracting vigorously, a situation that most commonly occurs when both the venous return is decreased and the sympathetic tone is high.

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Vasodepressor syncope tends to have characteristic clinical features that should lead the physician directly to the correct diagnosis. Many individuals tend to have a predisposition to vasodepressor syncope, so that episodes tend to recur periodically during a patient’s lifetime. The initial episode of syncope often occurs during the patient’s teen years. Over time, such individuals often have episodes that fall into several of the syndromes listed in Table 10.2. Vasodepressor syncope is most often preceded by at least a few seconds of prodromal symptoms (lightheadedness, ringing in the ears, visual disturbances, diaphoresis, and nausea are the most prominent) and occurs almost always when the patient is upright (sitting or standing). Syncope resolves almost immediately when the patient assumes the supine position (often by falling). The vasodilation tends to persist for several minutes, so that if the patient tries to get up immediately after such an episode, a second syncopal episode often occurs. A prolonged feeling of being “washed out” and being unable to function is common after vasodepressor syncope and is probably related to a residual autonomic imbalance triggered by the episode; unfortunately, these postdromal symptoms are often mistaken by clinicians for a “postictal” state. Patients who are predisposed to vasodepressor syncope will often have episodes of syncope when they are in a warm environment, when they have a viral illness, when they are dehydrated, or when they are under signiﬁcant stress. The syndromes related to cardiac C ﬁber stimulation are relatively uncommon in patients with signiﬁcant cardiac dysfunction, possibly because the C ﬁbers are affected by myocardial disease. Not uncommonly, patients prone to vasodepressor syncope will experience a ﬂurry of syncopal events over a period of days or weeks. Most often the reason for these ﬂurries is unclear. In some instances, however, such a ﬂurry may be a clue that the patient has developed an occult peptic ulcer or a urinary tract infection that predisposes to vasodepressor episodes. Obviously, given these prominent clinical features of vasodepressor syncope, taking a careful history is vitally important in making the correct diagnosis. As can be seen by studying Table 10.2, a patient’s activity at the time of syncope yields strong clues as to the mechanism. Syncope that occurs while micturating, defecating, coughing, or swallowing is almost always vasodepressor in origin. The same holds for syncope associated with fright, pain, noxious stimulation, or severe emotional stress. These syncopal episodes rarely cause a diagnostic dilemma, but obtaining a history of such episodes in the past may yield clues as to the etiology for more recent and less clear-cut episodes of vasodepressor syncope. Syncope that occurs immediately after stopping prolonged or vigorous exercise is usually vasodepressor in origin (as

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opposed to syncope that occurs during vigorous exercise). In the author’s experience, syncope that occurs in church (especially during the winter holidays, when tightly packed worshippers remain bundled in layers of cold-weather raiment) is usually due to a vasodepressor response. In a related phenomenon, syncope among members of the choir is also vasodepressor in origin in most cases. No other form of syncope is as situational as vasodepressor syncope.

Tilt table testing

In recent years, the upright tilt table study has entered common usage for determining a patient’s propensity to develop vasodepressor syncope. When subjected to an upright, motionless tilt, patients who have vasodepressor syncope will often develop a frank syncopal episode. The protocol used in performing tilt table testing varies among laboratories, but most centers tilt patients for 15–45 minutes at 60–85°. “Normal” individuals compensate for such a tilt by increasing both αand β-adrenergic tone as a result of baroreceptor stimulation and thus compensate for the decrease in venous return. In susceptible patients, however, these compensatory mechanisms eventually collapse. In such individuals, venous return is apparently never completely compensated. Thus, sympathetic tone progressively increases until, eventually, vigorous squeezing of the relatively empty ventricles results in recruitment of the cardiac C ﬁbers. This, in turn, causes stimulation of the medullary vasodepressor region. The result is a sudden withdrawal of sympathetic tone, a sudden increase in vagal tone, sudden vasodilation, and syncope. A positive tilt table study therefore identiﬁes a patient who is prone to vasodepressor syncope. The tile table study is positive in 30–74% of patients with syncope of unknown origin. Occasionally, however, an isoproterenol infusion is necessary to bring out syncope during tilt table testing, even in patients who, by history, clearly have vasodepressor syncope. Further, the reproducibility of tilt table testing has not been demonstrated, so that serial tilt table studies to measure the efﬁcacy of pharmacologic treatment are of questionable value. The tilt table study has been reported as being positive in up to 7% of individuals who do not have a history of syncope. Whether this represents a “false positive” response or a true propensity for vasodepressor syncope is unknown. It is likely, however, that aggressive upright tilting would eventually produce hemodynamic collapse in almost anybody — otherwise, cruciﬁxion would never have become a popular and effective form of execution.

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Treating vasodepressor syncope

The most effective form of therapy for vasodepressor syncope is educating the patient. The patient who has had one or more vasodepressor episodes should be advised as to the types of situations that predispose to vasodepressor syncope. Aggressive hydration should be advised when the patient is exercising, suffering from a viral illness or other infectious condition, or if he or she is working in a hot environment. The symptoms experienced by the patient before losing consciousness — the prodrome of vasodepressor syncope — should be stressed as a warning that syncope is imminent. The patient should be advised to immediately assume the supine position under such circumstances until the symptoms pass, in order to avoid losing consciousness. With such measures, especially in patients who have infrequent episodes, often no other therapy is necessary. Pharmacologic therapy for vasodepressor syncope is occasionally effective. Beta Blocking agents have recently become popular for treating vasodepressor syncope. Such therapy may seem paradoxical in a condition in which bradycardia is often a prominent feature, but because hypersympathetic tone is necessary to engage the cardiac C ﬁbers, there is some rationale for using β blockers. Disopyramide has also been used. Disopyramide has a vagolytic effect, but it also has a direct negative inotropic effect on the heart, and thus presumably inhibits stimulation of the cardiac C ﬁbers as well. Beta Blockers and disopyramide can be expected to be effective only when the patient experiences episodes of syncope that are mediated by the cardiac C ﬁbers, however. In addition, theophylline preparations, transdermal scopolamine, midodrine, ﬂudrocortisone, and ﬂuoxetine and other serotonin uptake inhibitors have been used with mixed success. Often, combinations of medications must be tried. Pharmacologic therapy should be reserved for patients who have frequent episodes of syncope and in whom nonpharmacologic methods have not been helpful. Because bradycardia alone is only rarely the proximate cause of syncope in the vasodepressor syndromes, pacemaker therapy prevents these episodes only rarely and is generally reserved for patients who have profound and prolonged bradycardia accompanying their episodes. If pacemaker therapy is to be used, a dual-chamber pacemaker should be implanted to maintain AV coordination during pacing.

Evaluation of the patient with syncope Classically, the evaluation of syncope has centered on searching for neurologic etiologies. During the past two decades, however, it has become

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apparent that most syncopal episodes have cardiovascular causes. The physician evaluating a patient with syncope should therefore search carefully for cardiovascular etiologies. Table 10.3 outlines a three-step approach for evaluating the patient with syncope. The most important step is to obtain a careful history and perform a physical examination. Although these steps are important in the evaluation of any medical condition, they are particularly important in the patient with syncope. The history yields important clues relative to the presence of neurologic conditions, underlying cardiac conditions, and vasodepressor syncope. The physical examination is important in uncovering the presence of occult neurologic lesions and cardiac disorders. When you approach the patient with syncope, your attitude must be that you will not leave the bedside until a presumptive diagnosis is clear; for once you decide that laboratory studies must be relied on to make the diagnosis, you’ve got a very difﬁcult task ahead. The ECG is important in the patient with syncope. The presence of Q waves, an intraventricular conduction abnormality, or ventricular arrhythmias should alert the physician to the presence of underlying cardiac disease that may predispose to lethal ventricular arrhythmias. Heart block or the presence of sinus bradycardia or sinus pauses all point to bradycardias as a potential etiology. A short PR interval or preexcitation indicates a bypass tract that may be the cause of syncope. The ECG should also be examined for repolarization abnormalities that may Table 10.3 Evaluation of the Patient with Syncope. Step 1 History and physical examination, ECG, serum electrolytes Step 2 (a) If neurologic problem suspected after step 1, consider an electroencephalography (EEG), brain scan, or angiography. (b) If vasodepressor syncope suspected, consider further work-up as necessary to rule out reversible lesions (e.g., gastrointestinal or genitourinary disease), and initiate therapy. Tilt table testing generally not necessary. (c) If cardiac disease is suspected or if cause remains unclear, do noninvasive cardiac work-up to assess ventricular function (echocardiogram). Where appropriate, consider treadmill testing or cardiac catheterization. Step 3 If the cause of syncope remains unclear after step 2: (a) If structural heart disease is present, do a full cardiac evaluation, then electrophysiologic testing (may do signal-averaged ECG as screening study before electrophysiologic testing). (b) If structural heart disease is absent, consider ambulatory monitoring, treadmill testing, and observation. If syncope recurs, consider tilt table testing and electrophysiologic testing.

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indicate a propensity for torsade de pointes or that may indicate underlying ischemic heart disease. The routine performance of brain scanning or electroencephalography (EEG) has not been helpful, and these tests should not be ordered unless the history or physical examination suggests a neurologic lesion or seizures. In cases in which a seizure has occurred but the EEG is negative, tilt table testing should be considered, because seizure-like activity can be reproduced by inducing vasodepressor syncope in some patients (thus sparing the patient the diagnosis of epilepsy). Tilt table testing is not necessary in patients with a classic history for vasodepressor syncope. In these patients, therapy for vasodepressor syncope is appropriate even if the tilt table study is negative. Exercise-related syncope is usually vasodepressor in origin in younger patients, but in older patients is more likely to be related to ventricular arrhythmias, especially if underlying cardiac disease is present. Even younger patients with exercise-related syncope should have treadmill testing, however, to look for exercise-induced arrhythmias, and echocardiograms to look for structural abnormalities that may produce syncope (especially hypertrophic cardiomyopathy). The most important, and the most neglected, part of the evaluation of syncope is to rule out underlying cardiac disease. In middle-aged and elderly patients with syncope, especially if syncope is of recent onset, a noninvasive evaluation of ventricular function is essential. An echocardiogram is probably the most useful means of assessing cardiac function because it also yields information relative to potential aortic outﬂow lesions. A signal-averaged ECG also may be performed as a screening study for ventricular arrhythmias in patients suspected of having underlying cardiac disease. Although arrhythmias are an important cause of syncope, ambulatory monitoring has generally been disappointing as a means of diagnosing arrhythmic syncope. A cardiac loop recorder (event recorder) can be helpful when symptomatic sinus nodal dysfunction or supraventricular tachycardia is suspected. When ventricular arrhythmias are suspected, however, ambulatory monitoring is inappropriate. Immediate electrophysiologic testing is indicated in patients with syncope of unknown origin who are found to have had a previous myocardial infarction, a depressed left ventricular ejection fraction, nonsustained ventricular tachycardia, or a positive signal-averaged ECG. These patients should be presumed to be at high risk for sudden death from ventricular arrhythmias until proven otherwise and should be hospitalized and monitored until ventricular arrhythmias are either ruled out or controlled.

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Electrophysiologic testing, usually in conjunction with tilt table testing, should be strongly considered when a careful noninvasive evaluation has failed to reveal a presumptive diagnosis for syncope. Such combined testing can yield a presumptive diagnosis in up to 74% of patients whose syncope was of unknown origin before testing. The evaluation of patients with syncope often has been regarded as difﬁcult and frustrating. Using the principles outlined in this chapter, however, a diagnosis can be made relatively quickly in the vast majority of patients presenting with syncope.

C H A P T E R 11

Electrophysiologic Testing in Perspective: the Evaluation and Treatment of Cardiac Arrhythmias

In this ﬁnal chapter, we will attempt to synthesize the information presented in the ﬁrst ten chapters into a general approach to the evaluation and treatment of cardiac arrhythmias, with emphasis on the appropriate use of the electrophysiology study. The approach outlined in this chapter is an elementary, and indeed, almost a trivial one. Quite simply, the basic principle of our approach is to tailor the aggressiveness of the therapy to the severity of the arrhythmia being treated. Nearly all serious mistakes that are made in the management of cardiac rhythm disturbances can be traced to a violation of this modest principle. Each year, thousands of patients die because their physicians tread lightly when faced with clearly lethal rhythm disturbances or, worse, become Ninja-like in their attack on benign arrhythmias. Such fatal mistakes can be avoided by taking a logical, stepwise approach to the evaluation and treatment of cardiac arrhythmias.

The three steps in evaluating and treating cardiac arrhythmias The appropriate management of cardiac arrhythmias involves following a predetermined plan of therapy aimed at achieving speciﬁc goals. Those goals, in turn, are determined by the severity of the arrhythmia being treated. Thus, in evaluating and treating cardiac arrhythmias, three discrete steps are implicit: Step 1. Assess the severity of the arrhythmia to be treated. The physician decides whether the arrhythmia is benign, potentially harmful, or lethal, and whether the symptoms associated with the arrhythmia require treatment. Step 2. Decide on the therapeutic end point. The physician decides whether the primary goal of treatment is to prevent death, to minimize harm, or merely to relieve symptoms. 278

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Step 3. Design the treatment plan. The physician devises a treatment plan that is directly aimed at achieving the primary therapeutic end point. Step 1 — Assess the severity of the arrhythmia to be treated

As already stated, the most common and most serious mistake made in the management of cardiac arrhythmias is to institute therapy that is inappropriate for the arrhythmia being treated. This error most often results from the propensity of physicians to assign speciﬁc treatments to speciﬁc arrhythmias, without considering the setting in which the arrhythmia occurs. Example: Dr. X uses ﬂecainide or encainide to treat all patients with premature ventricular contractions (PVCs; prior to 1990, this was an extremely common practice). For Patient A, who has a normal heart and asymptomatic complex ventricular ectopy, this therapy is too aggressive. Patient A has a normal risk of sudden death, and antiarrhythmic drugs cannot be expected to improve that normal risk (they may, on the other hand, increase the risk). For Patient B, who is a survivor of sudden cardiac death with PVCs, this therapy is not aggressive enough. Patient B has an extremely high risk of sudden death, and empiric therapy with ﬂecainide is not likely to help — indeed, the risk of proarrhythmia is especially high in such patients.

Physicians who treat a speciﬁc arrhythmia the same way in every patient will eventually cause serious problems because the appropriate treatment for an arrhythmia depends on more than just the arrhythmia itself. The appropriate level of aggressiveness in treating an arrhythmia can be judged only when considering the setting in which the arrhythmia occurs. In assessing the severity of a patient’s arrhythmia, the physician must consider at least three factors: 1) What is the arrhythmia? 2) What symptoms are associated with the arrhythmia? 3) What is the nature and the extent of any underlying cardiac disease? Several specialized laboratory studies are available to help assess these three factors. The studies most often used are those that help to assess the arrhythmia itself (the electrophysiology study and ambulatory monitoring) and those that help to assess underlying cardiac disease (cardiac catheterization, stress testing, echocardiography, and nuclear angiography). The electrophysiology study, as helpful as it is in guiding the therapy of many cardiac arrhythmias, is only modestly helpful in assessing the severity of arrhythmias. Because the arrhythmias induced in the electrophysiology laboratory are produced under unnatural circumstances,

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the electrophysiology study is poor at helping to correlate symptoms with arrhythmias. Observing symptoms with spontaneously occurring arrhythmias is far more helpful. On the other hand, in circumstances where an arrhythmia is suspected but not documented, the electrophysiology study can be helpful in diagnosing the arrhythmia itself. The most common example would be in patients with syncope of unknown origin (see Chapter 10). In such patients, the electrophysiology study can help to diagnose sinus node disease, distal conducting system disease, and ventricular tachyarrhythmias. It bears repeating, however, that both sinus node disease and conducting system disease can most often be diagnosed noninvasively. Regarding ventricular tachyarrhythmias, the sensitivity and speciﬁcity of induced ventricular arrhythmias in patients with syncope of unknown origin are strongly related to the presence and the extent of underlying heart disease. In general, electrophysiologic testing should be done in patients with syncope of unknown origin only when they have signiﬁcant heart disease or when there is a particular reason to suspect an arrhythmic etiology for syncope. The electrophysiology study, in addition, can help to assess the potential for developing severe arrhythmias in patients with atrioventricular bypass tracts (see Chapter 6). Except for patients with syncope of unknown origin or with bypass tracts, the electrophysiology study is, however, of limited usefulness in assessing the severity of arrhythmias. Ambulatory monitoring is often more helpful than electrophysiologic testing in assessing the severity of cardiac arrhythmias. In patients who are having reasonably frequent spontaneous arrhythmias, ambulatory monitoring is excellent in helping to correlate the arrhythmia with symptoms. Further, the speciﬁcity of spontaneous arrhythmias (as opposed to induced arrhythmias) is 100%. There are three general varieties of ambulatory monitoring. The Holter monitor study typically records the cardiac electrogram for 24 hours. If patients are having arrhythmias that occur at least daily, the Holter study is often ideal for assessing the severity of the arrhythmia because it gives information on the frequency of occurrence, potential exacerbating inﬂuences, and related symptoms. The second variety of ambulatory monitor, the cardiac event recorder, records the cardiac electrogram on a continuous tape, so that at any time only the last 30–90 seconds are available for playback. When a symptomatic arrhythmia occurs, the patient can stop the tape by pressing a button and then transmit the contents of the tape by telephone. Such a monitor is usually worn for extended periods of time, until a symptomatic episode is captured on tape. This type of monitor is best suited for a patient who has

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relatively infrequent symptomatic arrhythmias that have been difﬁcult to document. Finally, there is the implantable rhythm monitor. This is a tiny microprocessor-based device that is placed under the skin and records a patient’s ECG for weeks or months at a time. Rhythm strips from inside the device can be downloaded periodically and reviewed. Some electrophysiologists have found this device helpful in assessing the frequency and severity of benign (but symptomatic) cardiac arrhythmias. The implantable rhythm monitor has also been used to help diagnose syncope of unknown origin — but it must be stressed that it is inappropriate to rely on this form of ambulatory monitoring (or any ambulatory monitoring) to reveal arrhythmia-induced syncope, at least until ventricular arrhythmias either have been ruled out as the cause of syncope by electrophysiologic testing, or have been deemed as extremely unlikely after a noninvasive cardiac workup. (See Chapter 10.) The studies used to assess underlying heart disease will vary from patient to patient. Nuclear angiography and echocardiography are often used because these relatively noninvasive tests give excellent information on ventricular wall motion and left ventricular ejection fraction. The echocardiogram is especially useful when signiﬁcant valvular heart disease or hypertrophic cardiomyopathy are suspected. If cardiac ischemia is suspected, stress/thallium testing and cardiac catheterization are commonly used. What is the arrhythmia?

Diagnosing the arrhythmia of concern is an important ﬁrst step. Once the arrhythmia in question is known, some attempt should be made to classify the risk for sudden death imposed by the arrhythmia as low, moderate, or high. Such a classiﬁcation, based on the arrhythmia itself, is listed in Table 11.1. Note that some arrhythmias, by their very nature, should automatically be considered as imposing a high risk, namely, sustained ventricular tachycardia, ventricular ﬁbrillation, and complete heart block with an inadequate escape mechanism. The presence of atrial ﬁbrillation itself produces an increased risk of embolic stroke. Most other arrhythmias usually impose low or moderate risk, depending on the underlying heart disease. What symptoms are associated with the arrhythmia?

Arrhythmias generally cause only a few types of symptoms: Palpitations, lightheadedness or dizziness, or loss of consciousness. Palpitations are the most common symptom and are commonly associated with ectopic beats. Most patients can tolerate palpitations if this is the

282 II Electrophysiology Testing for Cardiac Arrhythmias Table 11.1 Classiﬁcation of the Risk for Sudden Death Imposed by Arrhythmias. High risk

Moderate risk

Low risk

Ventricular tachycardia

Complex ventricular ectopy with underlying heart disease

Premature atrial complexes

Ventricular ﬁbrillation Third-degree AV block with an inadequate escape Wolff-ParkinsonWhite Syndrome with rapid antegrade conduction in atrial ﬁbrillation

Second-degree AV block Third-degree AV block with adequate escape Atrial ﬁbrillation

Premature ventricular complexes Sinus node dysfunction Supraventricular tachycardias Complex ventricular ectopy with no underlying heart disease First-degree AV block

only symptom they experience, especially if they can be reassured that their arrhythmia is benign. Lightheadedness and dizziness, which occur with various levels of severity, tend to be associated either with bradyarrhythmias or with tachyarrhythmias that consist of more than isolated extra beats. Although many patients can tolerate occasional mild episodes of lightheadedness, others ﬁnd these symptoms to be extremely disturbing. Loss of consciousness from an arrhythmia indicates extreme hemodynamic compromise, and any bradyarrhythmia or tachyarrhythmia that produces this symptom should be considered to imply a high risk of sudden death. (An important exception to this rule: Syncope accompanied by bradycardias is most often vasoactive in nature. In these cases, the bradycardia itself is usually not the cause of syncope [instead, vasodilation is the cause] and should not be considered a lethal arrhythmia.) Some arrhythmias cause symptoms by producing or worsening symptoms of congestive heart failure. Any form of tachycardia that persists for weeks or months (such as persistent reentrant supraventricular tachycardia, inappropriate sinus tachycardia, or atrial ﬁbrillation with a rapid ventricular response) can ultimately produce ventricular remodeling and dilation and thus congestive heart failure. In patients with diastolic dysfunction, whose non-compliant ventricles are dependent on atrial contraction to achieve a high end-diastolic pressure while maintaining a relatively normal mean atrial pressure, loss of that atrial

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contraction with the onset of atrial ﬁbrillation can produce pulmonary congestion quite acutely. When a patient has symptoms compatible with an arrhythmia, determining whether those symptoms are actually due to an arrhythmia is not always straightforward. Quite often, a Holter monitor study will show arrhythmias and symptoms but will fail to show a correlation between the two. In these instances, the arrhythmia should not be construed as the cause of the symptoms. Because the appropriate treatment of many nonlethal arrhythmias depends on the symptoms they produce, every attempt should be made to document a correlation between the arrhythmia and the symptoms before any potentially toxic therapy is initiated. Further, several symptoms are often attributed to arrhythmias but in fact are only rarely due to arrhythmias. These symptoms include dyspnea, nonspeciﬁc fatigue, and seizures or localizing neurologic symptoms. Any of these symptoms, even if accompanied by cardiac arrhythmias, should prompt a thorough search for other causes. Once it is determined that symptoms are due to the arrhythmia in question, those symptoms should be categorized in terms of their severity. The classiﬁcation of the severity of symptoms described in Table 11.2 includes three categories: Life-threatening symptoms, severely disruptive symptoms, and minor or no symptoms. What is the underlying heart disease?

In general, any arrhythmia is more severe in the face of signiﬁcant underlying heart disease than with a normal heart. In particular, as described in Chapter 7, underlying heart disease is the primary determinant of lethal ventricular arrhythmias. Thus, complex ventricular ectopy that has no signiﬁcance in a patient with no heart disease, has signiﬁcant implications in patients with severe left ventricular dysfunction. By considering these three factors, one can accurately judge the severity of the arrhythmia in question. The next step is to use this information to decide on a speciﬁc goal of therapy. Table 11.2 Classiﬁcation of the Severity of Arrhythmic Symptoms. Life-threatening: presyncope, syncope, or aborted sudden death Severely disruptive: signiﬁcant lightheadedness or dizziness, severe palpitations, worsening congestive heart failure (such as in atrial ﬁbrillation with rapid ventricular response) Minor/none: mild lightheadedness, palpitations

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Step 2 — Decide on the therapeutic end point

Cardiac arrhythmias are treated either because they produce symptoms, pose a threat to health, or have the potential to cause sudden death. Thus, there are three general therapeutic end points in treating cardiac arrhythmias: To relieve symptoms, to maintain health, or to prevent sudden death. Before a treatment plan can be devised, it is vital to decide which of these goals is to be pursued and to keep that goal clearly in mind. The appropriate goal of therapy should be chosen based on the severity of the arrhythmia, as determined in step 1. The following generalizations can be made. Low-risk arrhythmias, because they do not have the potential to produce death, should be treated only if they are producing symptoms that are disruptive to the patient’s life, in which case the goal of therapy is merely to reduce symptoms. High-risk arrhythmias, on the other hand, should always be treated, and the goal of therapy with these arrhythmias is to prevent sudden death. Moderate-risk arrhythmias are the most problematic. Two arrhythmias tend to fall in to this category: Atrial ﬁbrillation and complex ventricular ectopy in the setting of signiﬁcant underlying cardiac disease. Atrial ﬁbrillation presents a problem (aside from the symptoms caused by the arrhythmia itself) because it poses a long-term risk of embolic stroke, and in some patients it can produce or exacerbate heart failure. Furthermore, as we have discussed, “getting rid” of atrial ﬁbrillation (with either antiarrhythmic drugs or ablation) can be extremely difﬁcult and risky. So, in treating this arrhythmia the clinician must decide whether to use a “conservative” approach (controlling the rate response and anticoagulating), or an “aggressive” approach (trying to restore and maintain sinus rhythm). Neither of these approaches is easy or straightforward, and both may require escalating attempts at achieving the therapeutic goal (for instance, advancing from drug-based therapy to ablation-based therapy). Complex ventricular ectopy, in the setting of signiﬁcant underlying cardiac disease, has become much less a clinical dilemma than it used to be, for two reasons. First, it is now well established that trying to abolish these arrhythmias with antiarrhythmic drugs merely increases risk, and that treating empirically with amiodarone does not improve outcomes. So the temptation to treat the ectopy itself has become much less compelling. And second, as described in Chapter 7, thanks to the results of several randomized clinical trials, we can now offer implantable deﬁbrillators to many of these patients. So, while treatment still does not entail getting rid of the ectopy itself, we are now able to materially improve the survival of many of the patients who fall into this category.

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Step 3 — Design the treatment plan

The ﬁnal step in the management of cardiac arrhythmias is to decide on a therapeutic plan aimed at achieving the chosen goal of therapy. Keeping the goal of therapy clearly in mind is vitally important because treatments for similar arrhythmias may vary markedly from patient to patient, depending on whether the aim of therapy is to prevent sudden death or merely to relieve symptoms. (It should be noted that in managing bradyarrhythmias, the basic therapy for both relieving symptoms and preventing sudden death is essentially the same — a permanent pacemaker. The following discussion then pertains mainly to ectopic beats and tachyarrhythmias.) Treating to relieve symptoms

When the primary goal of therapy is to relieve symptoms, the physician must determine what steps are necessary to achieve that goal. For most patients in whom symptom relief is the therapeutic end point, the arrhythmia being treated is benign. Thus, therapy aimed at relieving symptoms is often (and appropriately) less aggressive than therapy aimed at preventing sudden death. Empiric trial-and-error therapeutic attempts are often appropriate and are frequently performed on an outpatient basis. Generally, milder therapies are tried ﬁrst, moving progressively and as necessary to more aggressive treatments. Before each escalation of therapy, careful consideration is given as to whether the symptom being treated warrants yet more aggressive therapy. Although serial ambulatory monitoring is often helpful, it should be remembered that, when the goal is merely to relieve symptoms, the therapeutic goal has already been met if monitoring is necessary to tell whether the arrhythmia is still present. The level of aggressiveness used in controlling symptoms depends on the severity of the symptoms being treated. For instance, therapy to relieve symptoms does not necessarily involve suppressing the culprit arrhythmia. Quite often, the symptoms that a patient experiences with a benign arrhythmia are magniﬁed by the anxiety that often accompanies the knowledge that one has a cardiac arrhythmia (an anxiety that is often provoked by a physician, who expresses grave concern over the arrhythmia’s presence). In such cases, the symptoms often can be ameliorated simply by reassuring the patient of the benign nature of the arrhythmia. The therapeutic goal of relieving symptoms, then, can sometimes be achieved without subjecting the patient to potentially toxic drugs, and without affecting the frequency of the offending arrhythmia at all.

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On the other hand, a patient may have an arrhythmia that is non–lifethreatening but that produces severely disabling symptoms. In such instances, it may be entirely appropriate to attempt very aggressive therapy. As an example, consider a patient with severe cardiomyopathy who has atrial ﬁbrillation with a rapid ventricular response, resulting in moderate decompensation of the patient’s congestive heart failure. With such a patient, one might begin with attempts to control the ventricular response with digitalization, calcium blockers, or β blockers. If this were unsuccessful, one would have to consider more radical measures, such as His bundle ablation and insertion of a permanent pacemaker. Therefore, one may arrive at aggressive therapy in relieving the symptoms of an arrhythmia, but in general only after less aggressive measures have failed. The electrophysiology study has only a moderate role in managing arrhythmias when the suppression of symptoms is the primary goal. Although the electrophysiology can help in assessing the presence of various nonlethal arrhythmias (such as sinus node or AV node dysfunction), this study cannot supply much information on the symptoms caused by these arrhythmias. For several types of arrhythmias, however, the electrophysiology study can be helpful in abolishing symptoms. This is especially true for most reentrant supraventricular tachycardias, which usually can be cured with transcatheter ablation. Treating to prevent sudden death

Once the physician decides that the primary goal of therapy is to prevent the patient’s sudden death, a treatment plan should be devised that reﬂects the urgency of the therapeutic end point. By its nature, sudden death occurs instantaneously and unexpectedly. Thus, when a patient is judged to be a candidate for sudden death, immediate and aggressive efforts should be made to prevent this event. Ideally, these efforts should include placing the patient in the hospital and on a monitor until adequate therapy is derived. Trial-and-error (empiric) methods of treatment are inappropriate. When the goal of therapy is to prevent sudden death, the initial therapy must be effective because the physician is unlikely to have a second chance should therapy prove ineffective. With regard to patients who are at high risk for sudden death from ventricular arrhythmias, the treatment “plan” has been greatly simpliﬁed over the past few years. In contrast to the days when the electrophysiology study was used as the cornerstone of a complex therapy-selection strategy, today the “baseline” treatment strategy is almost always the same — to insert an implantable deﬁbrillator. The electrophysiology

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287

study, when done at all, is generally used to help determine how to optimally program the implantable deﬁbrillator — for instance, in optimizing antitachycardia pacing. For the other major variety of arrhythmia that poses an increased risk of sudden death — a bypass tract with rapid antegrade conduction — the electrophysiology study with ablation remains the mainstay of effective treatment.

Summary This ﬁnal chapter outlines a general approach to, and a perspective on, the use of the electrophysiology study in the management of cardiac arrhythmias. Devising a reasonable treatment plan depends on deﬁning the goals of therapy. Those goals, in turn, depend on the severity of the arrhythmia and of the symptoms caused by the arrhythmia. The electrophysiology study can be of moderate help in assessing the severity of cardiac arrhythmias and can be extremely helpful in abolishing both the symptoms and the risk caused by several cardiac arrhythmias. Most fatal mistakes in treating cardiac arrhythmias stem from failing to match the aggressiveness of therapy to the severity of the arrhythmia being treated. Using a logical, stepwise approach to the evaluation and treatment of cardiac arrhythmias allows one to avoid this critical error.

Index

Note: page numbers followed by f refer to ﬁgures, those followed by t refer to tables. AV, atrioventricular; ECG, electrocardiogram; SA, sinoatrial. A deﬂection, 79, 80f A spike, 47f, 49 AAI pacemakers, 95–97 AAIR pacemakers, 96, 101–102 Ablation/ablative techniques, 31 atrial ﬁbrillation, 152, 236–239 atrial ﬂutter, 234–236, 234f, 235f atrial tachycardias, focal, 233 atrioventricular (AV) junction, 214–216, 215f bypass tracts See Bypass tract ablation His bundle, 214–215, 215f radiofrequency See Radiofrequency ablation radiofrequency vs. direct current (DC) shock, 213–214 sinoatrial (SA) node, 70, 72 transcatheter See Transcatheter ablation ventricular tachycardia, 247–250 idiopathic, 247–248 reentrant, 195, 240–246 N-Acetylprocainamide, 26 Action potential, 5–8, 6f antiarrhythmic drug effects, 23, 24f depolarization See Depolarization localized differences, 9, 9f repolarization, 7, 11 resting phase, 7–8, 8f surface ECG relationship, 10f, 11 Activation mapping, 241f, 242–243, 247 Adenosine, 169, 229 AFFIRM trial, 153 Afterdepolarizations, 20, 21f delayed, 187f, 190 early, 186, 187f, 188f triggered activity ventricular arrhythmias, 186, 187f AH interval, 47f, 49–50, 50, 79, 81 ﬁrst-degree AV block, 81, 81f prolongation in second-degree AV block, 82–83 supraventricular tachycardia, 114–115 Ambulatory monitoring, 270, 276, 280–281 American College of Cardiology, 193, 257 American Heart Association, 257

288

Amiodarone, 26 macroreentrant supraventricular tachycardia, 142 toxicity, 29 ventricular arrhythmias, 195, 196t Anatomy AV node, 217f, 218 cardiac electrical system, 3–5, 4f SA node, 59 Anteroseptal bypass tracts, 138–139 ablation, 231–233, 232f Antiarrhythmic drugs, 22–30 See also speciﬁc drugs automatic tachycardia induction, 15 class I, 24, 25t action potential effects, 24f mechanism of action, 22–23, 23f class Ia, 24, 25t atrial ﬁbrillation, 144, 152 atrial ﬂutter, 150 automatic supraventricular tachycardias, 105 AV nodal bypass tracts, 145 AV nodal reentry, 129 contraindications, 27 intraatrial reentry, 108, 147 macroreentrant supraventricular tachycardia, 142 proarrhythmia risk, 29, 30t reentrant supraventricular tachycardia, 119 reentrant tachycardias, 26, 28f class Ib, 24, 25t, 26 contraindications, 27 proarrhythmia risk, 30t reentrant supraventricular tachycardia, 119 reentrant tachycardias, 26, 28f class Ic, 25t, 26 atrial ﬁbrillation, 144, 152 atrial ﬂutter, 150 AV nodal bypass tracts, 145 AV nodal reentry, 129 inappropriate sinus tachycardia, 72 intraatrial reentry, 147 macroreentrant supraventricular tachycardia, 142 proarrhythmia risk, 30t reentrant supraventricular tachycardia, 119

Index 289 class II, 24f, 25t, 26 class III, 25t, 26 action potential effects, 24f atrial ﬁbrillation, 144, 152 atrial ﬂutter, 150 intraatrial reentry, 147 proarrhythmia risk, 29, 30t class IV, 24f, 25t, 26 class V, 25t, 26 classiﬁcation, 24–26, 25t effect of, 26–27, 28f mechanisms of action, 22–23, 23f proarrhythmic effect, 27, 29, 30t reentrant arrhythmias, 55–56 reentrant ventricular arrhythmias, 181 side effects, 31t toxicity, 29–30, 30t, 31t Antitachycardia pacing (ATP), 183–184 Anxiety, 285 Arrhythmias, 12–21 See also speciﬁc types ambulatory monitoring, 270, 276, 280–281 diagnosis, 281 exacerbation (proarrhythmia), 27, 29, 30t sudden death risk classiﬁcation, 281, 282t symptoms, 281–283 severity classiﬁcation, 279–283, 283, 283t three step evaluation/treatment plan, 278–287 treatment, 22–32 ablation See Ablation/ablative techniques device therapy, 31–32 nonpharmacologic, 30–32 pharmacologic See Antiarrhythmic drugs plan design, 279, 285–287 surgical, 31 therapeutic endpoints, 284 underlying cause reversal, 30 underlying heart disease, 283 Atria See also entries beginning atrial electrode catheter positioning in, 43–44 incremental pacing, 87–88 Atrial deﬁbrillation, 152 Atrial ﬁb-ﬂutter, 149–150 Atrial ﬁbrillation brady-tachy syndrome, 60–61 bypass tracts, 121, 143–144, 143f chronic, 150 electrophysiologic study in, 148, 150–154 functional refractory period, 52 paroxysmal/recent onset, 150, 154 risk classiﬁcation, 284 supraventricular tachycardias, 121 reentrant, 108–109, 109f treatment, 151–154 ablative, 152, 236–239 pacemakers, 96, 100 rate control, 152, 153–154 rhythm control, 151–152, 153–154 Atrial ﬂutter atypical, 236 bypass tracts, 143–144 electrophysiologic study in, 148–150, 149f reentrant supraventricular tachycardias, 108–109, 108f treatment, 150 ablative, 234–236, 234f, 235f Atrial myocardium, 128 Atrial pacing, 149 Atrial tachycardia ablation of, 233–239 multifocal, 104, 105f pacemaker mode switching, 97 Atrial thrombi, 151

“Atrial wavefront” model, 236–237 Atrioventricular (AV) block, 12–14, 73–74 automatic atrial tachycardia, 104 classiﬁcation of, 13, 14f complete, 77, 78, 78f, 251 distal, 89, 91f ﬁrst-degree, 13, 74, 75f His bundle electrogram of, 81–82, 81f intermittent, 75 localizing, 13–14, 78–79, 80f, 80t second-degree, 13, 75–76, 76f, 77f His bundle electrogram of, 82–83, 83f localization, 78 type I See Mobitz type I block (Wenckebach block) type II See Mobitz type II block syncope, 268 third-degree, 13, 77, 78f His bundle electrogram, 83, 84f treatment, 78, 79t 2 : 1 AV block, 76, 77f, 79, 108 Atrioventricular (AV) bypass tracts, 130, 131f, 132f Atrioventricular (AV) conduction block See Atrioventricular (AV) block disorders, 73–90 AV bypass tract reentrant tachycardia, 138, 139f AV nodal reentrant tachycardia, 126, 127f electrophysiologic study of, 79–90 inapparent, 83–89 overt, 81–83, 81f, 82f, 83f, 84f pacemaker indications, 93 site of, 73–74 supraventricular tachycardia, 114, 115f symptoms, 73 His bundle electrogram, 45 normal, 114–115, 115f slow, 9 Atrioventricular (AV) dissociation, 77, 78f Atrioventricular (AV) groove, 3–4, 130 Atrioventricular (AV) interval, 262 Atrioventricular (AV) junction, ablation, 214–216 direct current shock, 214, 215f radiofrequency energy, 214–216 Atrioventricular (AV) nodal reentrant supraventricular tachycardias, 106, 107f, 121–130 Atrioventricular (AV) nodal reentrant tachycardia, 216–221, 217–219f, 221f activation patterns, 126–128, 127f atrial/ventricular myocardium involvement, 128 atypical, 129 initiation, 123–125, 124f, 126f mechanism of reentry, 122–123, 122f P wave, 128–129, 155, 156f QRS complex, 128–129 supraventricular, 106, 107f, 121–130 termination, 123–125 treatment, 129–130 Atrioventricular (AV) node, 4 action potential, 9, 9f anatomy and physiology, 216, 217f, 218 autonomic innervation, 10 bypass tracts of, 130–131, 131f, 144–145 conduction See Atrioventricular (AV) conduction depolarization, 49 effective refractory period, 85, 86–87, 87f Atrium See Atria

290

Index

Automatic supraventricular tachycardias, 104–105, 105f Automatic ventricular arrhythmias, 160t, 184–185 Automaticity, 7–8, 8f autonomic innervation inﬂuence, 9–10 electrophysiologic evaluation, 47–48 programmed stimulation, 39 SA node assessment, 47–48 SA node insufﬁciency, 12 tachycardias See Tachycardias, automatic Autonomic blockade, 68 Autonomic maneuvers, 89 AV block localization, 79 AV nodal reentry, 129 reentrant arrhythmias, 55–56 supraventricular tachycardias, 118 Autonomic nervous system automaticity inﬂuence, 9–10 dysautonomia, 70–72 localized differences, 9–10 SA node, 59 Autonomic tone, 52 AV See entries beginning atrioventricular Baseline recording, 45, 47f supraventricular tachycardias, 111f Basic cycle length, 47f, 50, 64, 67 Baye’s theorem, 175 Beta blockers, 25t, 26 atrial ﬁbrillation, 144, 152 AV nodal reentry, 129 inappropriate sinus tachycardia, 72 SA nodal reentry, 148 supraventricular tachycardia, macroreentrant, 141 vasodepressor syncope, 274 ventricular tachycardia catecholamine-dependent, 56 idiopathic left, 191 outﬂow tract, 191 Bilateral fascicular block, 93 Bipolar recording conﬁguration, 38 Biventricular pacing See Cardiac resynchronization therapy (CRT) Bradyarrhythmia See Bradycardia Bradycardia, 12–14 AV conduction, 12, 73 See also Atrioventricular (AV) block impulse generation failure, 12, 13f impulse propagation failure, 12–14, 14f pacemakers in, 31–32 SA node dysfunction, 59 sinus See Sinus bradycardia syncope and, 266–268 Brady-tachy syndrome, 59, 60–61 Bretylium, 26 Brugada syndrome, 192 Bundle branch block, 58, 91–93 left, 92–93, 264 reentrant supraventricular tachycardia, 118, 119f right, 91–92 surface ECG effects, 11 ventricular dyssynchronyand, 254, 255f, 256 Bundle branch reentrant tachycardia, ablation, 248–250, 249f Bundle branch reentry, 192, 248–250 Burst pacing See Incremental (burst) pacing Bypass tract ablation, 222–233 anteroseptal, 231–233, 232f left free wall, 226–227 midseptal, 231–233, 232f

paraseptal, 229–231, 230f posterior septal, 229–231, 230f right free wall, 227–228, 228f Bypass tracts, 130 ablation See Bypass tract ablation antegrade conduction, 131 anterior septal, 138–139 atrial ﬁbrillation and, 143–144, 143f atrial ﬂutter and, 143–144 atrioventricular/AV nodal, 130–131, 131f, 132f, 144–145 characteristics of, 222 concealed, 133, 135–136, 137f electrophysiologic studies, 157 fasiculoventricular, 132f localization/mapping, 142–143, 224–226, 225f, 226f ECG, 222–224, 223f, 223t, 224t Mahaim, 131, 131f, 145, 228–229 multiple, 145–146 retrograde activation, 117f, 138 retrograde conduction, 133 supraventricular tachycardia See under Supraventricular tachycardias surgical treatment of, 146 types, 144–146 Calcium channel blockers, 25t, 26 atrial ﬁbrillation, 152 AV nodal reentry, 129 inappropriate sinus tachycardia, 72 SA nodal reentry, 148 supraventricular tachycardia, macroreentrant, 141 triggered activity tachycardias, 20 ventricular tachycardia idiopathic left, 191 outﬂow tract, 191 Calcium channels, 7, 20 Cardiac action potential See Action potential Cardiac Arrhythmia Suppression Trial (CAST), 194 Cardiac C ﬁbers, 271, 272 Cardiac electrical system, 3–11 action potential See Action potential anatomy, 3–5, 4f localized variations, 8–10 Cardiac emergency equipment, 41–42 Cardiac event recorder, 280–281 Cardiac ischemia, 31, 161, 190 Cardiac loop recorder, 276 Cardiac monitoring, SA node dysfunction, 68 Cardiac perforation, radiofrequency ablation risk, 251 Cardiac resynchronization therapy (CRT), 100, 253–265 clinical studies, 257, 258t complications, 259 contractility, 256 device implantation, 259 effectiveness of, 264–265 effects of, 256–257 hemodynamic effects, 256 indications for, 94, 257 left bundle branch block, 93 mechanism of action, 254–256, 255f non-responders, 260–261 optimization, 261–263 AV interval, 262 dyssynchrony measurement, 263 lead placement/number, 263 V-V interval, 262–263 rationing, 260

Index 291 responders, 260–261 reverse modeling, 256–257 ventricular arrhythmias, 210 Cardiac tamponade, radiofrequency ablation risk, 251 Cardiomyopathy, 286 Cardioneurogenic syncope See Vasodepressor syncope CARE-HF trial, 257, 258f, 261 CAST trial, 194 Catechol-dependent triggered activity ventricular tachycardias, 56, 186, 187f, 190 Catheterization, risks of, 56–57 Chronic fatigue syndrome (CFS), 71, 72 COMPANION trial, 257, 258f Complications, electrophysiologic study, 56–57 Concealed conduction, 135–136 Conduction , AV node See Atrioventricular (AV) conduction Conduction interval, 48–49 Conduction velocity, 7 cycle length, impact of, 52 electrophysiologic evaluation, 46f, 48–50 Congestive heart failure, 282 Consciousness loss See Syncope Coronary bypass surgery, 31 Coronary sinus diverticulum, 231 electrode catheter positioning in, 43–44, 44f Corrected sinus node recovery time (CSNRT), 64 Coupling interval, 36, 36f Crista terminalis, 59 Cycle length, 35–36, 36f basic, 47f, 50, 64, 67 conduction velocity impact, 52 refractory period impact, 52 DAVID trial, 264 DC cardioversion See Direct current (DC) cardioversion DC shock See Direct current (DC) shock DDD pacemakers, 97–100, 101 DDD pacing, 97–100, 98f mode switching, 97 pacemaker tachycardia, 97–100, 99f DDDR pacemakers, 97–100, 101, 264 Deﬁbrillation, atrial, 152 Deﬁbrillator in Acute Myocardial Infarction Trial (DINAMIT), 200–201, 210 Deﬁbrillators, implantable See also Implantable cardioverter-deﬁbrillator (ICD) atrial ﬁbrillation, 152 bundle branch reentrant tachycardia, 250 complex ventricular ectopy, 284 ventricular arrhythmias and, 286–287 Delayed afterdepolarizations (DADs), 187f, 190 Delta waves anteroseptal bypass tracts, 231–232 bypass tract localization, 222, 223f, 224 multiple bypass tract indication, 146 Depolarization, 6–7, 7–8 conduction velocity association, 48 intracardiac recording, 38–39 spontaneous, 8 See also Automaticity surface ECG effects, 11 Device therapy, 31–32 See also speciﬁc devices reentrant arrhythmias, 55–56 Digitalis, 25t, 26 atrial ﬁbrillation, 144, 152 atrial tachycardia, 104, 105 AV nodal reentry, 129 delayed afterdepolarizations, 190

macroreentrant supraventricular tachycardia, 141 SA nodal reentry, 148 toxicity, 104, 105, 190 Digitalis-toxic supraventricular arrhythmia, 21 Direct current (DC) cardioversion atrial ﬁbrillation, 151–152 reentrant ventricular arrhythmias, 176, 178 Direct current (DC) shock, 212 radiofrequency ablation versus, 213–214 Disopyramide, 24, 25t, 274 Dizziness, 282 Dofetilide, 26 Dysautonomia, 70–72 Early afterdepolarizations (EADs), 186, 187f, 188f ECG See Electrocardiogram (ECG) Echocardiogram, 276, 281 Effective refractory period (ERP), 50–51, 51f AV node, 85, 86–87, 87f His-Purkinje, 85–86, 87 reentrant arrhythmias, 53 supraventricular tachycardia initiation, 112–113 Electroanatomical mapping, 250 Electrocardiogram (ECG) AV block localization, 78 cardiac action potential relationship, 10f, 11 intracardiac electrogram association, 37–38, 38f PR interval, 4 signal-averaged See Signal-averaged surface ECG supraventricular tachycardias, 154–155 syncope, 275–276 Electrode catheters, 36–37, 37f bundle branch block, 92, 93 insertion, 42–45 positioning, 42–45, 44f, 46f atrial ﬂutter ablation, 235, 235f His bundle electrogram, 45, 46f left free wall bypass tract ablation, 227 posterior septal/paraseptal bypass tract ablation, 231 reentrant tachycardia, 53 right free wall bypass tract ablation, 227 supraventricular tachycardia, 43 supraventricular tachycardias, 110 ventricular pacing, 43 quadripolar, 37, 37f Electroencephalography (EEG), 276 Electromagnetic mapping, 250, 251 Electrophysiologic studies, 35–57 See also speciﬁc techniques/indications arrhythmia evaluation/treatment, 278–287 AV conduction disorders, 79–90 baseline recording, 45, 47f complications, 56–57 coupling interval, 36, 36f cycle length See Cycle length electrode catheters See Electrode catheters heart property evaluation, 47–52 intracardiac electrogram recording, 37–39, 38f laboratory setup, 40–42, 41f pacemaker selection, 101–102 pacing, 39, 40f patient preparation, 42 performance of, 40–46 protocol, 45–46 recording, 35–40 Encainide, 25t, 26, 194, 279 Entrainment mapping, 245–246

292

Index

Epicardial mapping, 250 Equipment, 40–42 Escape pacemakers, 14, 74 third-degree AV block, 77 Exercise-related syncope, 276 Extrastimulus pacing, 39, 40f AV conduction disorders, 84–87, 85–86f reentrant supraventricular tachycardia, 120 reentrant ventricular arrhythmia, 177, 177f Fasiculoventricular bypass tracts, 132f Flecainide, 25t, 26, 142, 194, 279 Focal atrial tachycardias, ablation, 233 Framingham study, 203 Functional refractory period (FRP), 51–52, 85 Gulf War syndrome, 72 H spike, 47f, 49, 79, 80f ﬁrst-degree AV block, 81 Health maintenance goal, 284 “Heart attack” See Myocardial infarction Heart block See Atrioventricular (AV) block Heart disease, 283 Heart failure cardiac resynchronization therapy indication, 257 implantable cardioverter-deﬁbrillator indication, 201 Heart rate, 35–36 Heart Rhythm Society, 193, 257 Heart rhythms, abnormal See Arrhythmias His bundle, 4, 4f ablation direct current shock, 214, 215f radiofrequency, 214–215 electrogram, 45, 80f AV conduction disorder evaluation, 79–81 conduction velocity measurement, 46f, 49 electrode catheter positioning, 45, 46f split, 81–82, 82f His-Purkinje system, 4 block, 73, 74, 89 See also Bundle branch block conduction time, 81 dysfunction, 87, 88f effective refractory period, 85–86, 87 Mobitz type II block, 83 Holter monitor, 280, 283 HV interval, 47f, 49, 50, 81 prolongation, 81, 81f, 82, 82f Ibutilide, 26 Idiopathic left ventricular tachycardia, 191 ablation, 247–248 Implantable cardioverter-deﬁbrillator (ICD) axiom of overall survival, 203–204, 205, 206–207t Brugada syndrome, 192 cost, 203, 204–209, 206–207t high-risk patients, 209 patient selection, 205 randomized trial drawbacks, 202–203 rationing, 204–205, 207 ventricular arrhythmias, 195–196 evidence-based approach, 197–209 indications for, 201 malignant tachycardia, 32 primary prevention trials, 198–201, 199t reentrant, 178, 183–184 secondary prevention trials, 198, 198t Implantable rhythm monitor, 281

Inappropriate sinus tachycardia (IST), 58, 69–73, 104–105 etiology, 70–72 symptoms, 69 treatment, 72–73 Incremental (burst) pacing, 39 AV conduction disorders, 87–89, 89–90f, 91f normal response, 88, 89–90f reentrant supraventricular tachycardia, 120 reentrant ventricular arrhythmia termination, 177, 177f Intraatrial conduction interval, 47f, 50 Intraatrial reentrant supraventricular tachycardias, 107–108, 107f, 155, 156, 156f Intraatrial reentry, electrophysiologic study, 146–147 Intracardiac electrogram bypass tract mapping, 142–143 recording, 37–39, 38f supraventricular tachycardia, 55 surface ECG association, 37–38, 38f Intraventricular conduction delay (IVCD), 91, 263 Ischemic heart disease, 31, 190 reentrant ventricular arrhythmias, 161 Isoproterenol infusion atrial ﬁbrillation in bypass tracts, 144 reentrant ventricular tachycardia, 171 right ventricular outﬂow tract tachycardia induction, 247 tilt table testing for vasodepressor syncope, 273 triggered activity ventricular arrhythmias, 190 Jervell-Lange-Nielson syndrome, 190 Junction box, 41 Junctional escape (JE) pacemakers, 14, 74 Koch’s triangle, 218–219, 218f, 219f Laboratory setup, 40–42, 41f Left bundle branch block (LBBB), 92–93, 264 Left free wall bypass tract ablation, 226–227 Left posteroseptal tachycardia See Idiopathic left ventricular tachycardia Lidocaine, 24, 25t, 26 Lightheadedness, 282 Macroreentrant supraventricular tachycardias See Supraventricular tachycardias, macroreentrant Magnesium sulfate, 189 Magnetic resonance imaging (MRI), 263 Mahaim bypass tracts, 131, 131f, 145, 228–229 Malignant ventricular tachycardia, 32 Mapping, 250–251 AV nodal reentrant tachycardia ablation, 220, 221f bypass tracts, 142–143, 224–226, 225f, 226f reentrant ventricular tachycardia, 240–246, 241f, 243–245f “Maze” procedure, 237–238 Mexiletine, 24, 25t Midseptal bypass tract ablation, 231–233, 232f Mitral valve prolapse, ventricular arrhythmia association, 193 Mobitz type I block (Wenckebach block), 75, 76f, 78, 79 His bundle electrogram, 82–83, 83, 83f incremental pacing, 88–89, 90f

Index 293 Mobitz type II block, 75, 76f, 78 His bundle electrogram, 83, 84f location, 83 Modiﬁed Seldinger technique, 42–43 Moricizine, 25t, 194 MOST trial, 264 Multicenter Autonomic Deﬁbrillation Implantation Trial (MADIT I), 199–200, 209 Multicenter Autonomic Deﬁbrillation Implantation Trial (MADIT II), 200, 209, 210 Multicenter Unsustained Tachycardia Trial (MUSTT), 200, 210 Myocardial contraction, electrical impulses of, 5 Myocardial ﬁbrosis, 162, 269 Myocardial infarction, 93 automatic ventricular arrhythmias, 185 implantable cardioverter-deﬁbrillator indication, 201 proarrhythmic effect of antiarrhythmics, 27 reentrant ventricular arrhythmias, 161, 163 transmural, 11 Narula method, 67 Neurasthenia, 70–71 Noncontact mapping, 250–251 Nuclear angiography, 281 Outﬂow tract ventricular tachycardia, 191 Overdrive suppression SA node, 61, 63 automaticity assessment, 47–48 supraventricular tachycardia and syncope, 268 P wave, 50 AV dissociation, 77, 78f AV nodal reentrant tachycardia, 128–129, 155, 156f depolarization representation, 11 supraventricular tachycardias, 155, 156f Pacemaker cells, subsidiary, 13, 14f overdrive suppression, 48 Pacemaker syndrome, 96–97, 100 Pacemaker tachycardia, 97–100, 99f Pacemakers (artiﬁcial), 93–102, 253 See also Cardiac resynchronization therapy (CRT); Pacing AAI, 95–97 AAIR, 96, 101–102 atrial ﬁbrillation, 152 automatic tachycardias, 56 bradycardia, 31–32 bundle branch block, 93 DDD, 97–100, 101 DDDR, 97–100, 101 dual-chambered, 94, 97–100, 100, 253 indications for, 93–94 macroreentrant supraventricular tachycardia, 142 mechanism of action, 31–32 nomenclature, 94–95 pacing modes, 95–100 rate-responsive, 95 See also speciﬁc types selection of, 100–102, 101f single-chambered, 94, 95–97, 100 tachycardias, 32 temporary placement, 48 vasodepressor syncope, 274 VVI, 95–97, 96f VVIR, 96 Pace-mapping, 245, 247

Pacing, 39, 40f See also Cardiac resynchronization therapy (CRT); Pacemakers (artiﬁcial) AAI, 95–96 atrial, 149 atrial ﬁb-ﬂutter, 150 atrial ﬂutter, 149 biventricular See Cardiac resynchronization therapy (CRT) burst See Incremental (burst) pacing cardiac resynchronization therapy (CRT), 100 DDD See DDD pacing DDDR, 264 extrastimulus See Extrastimulus pacing incremental See Incremental (burst) pacing rate-responsive, 95 reentrant tachycardia, 53, 55 reentrant ventricular tachycardia, 171 termination, 177, 177f sinus node recovery time measurement, 61, 63 supraventricular tachycardia, 55 ventricular See Ventricular pacing VVI, 95–97, 96f Palpitations, 281–282 Paraseptal bypass tract ablation, 229–231, 230f Parasympathetic tone automaticity effect, 9–10 conduction velocity effect, 52 reentrant supraventricular tachycardia, 118 refractory period effect, 52 Paroxysmal atrial tachycardia (PAT), 106–108, 109, 121 P wave, 155, 156f Patient preparation, 42 Pause-dependent triggered activity ventricular arrhythmias, 186–190, 187f, 188f, 189f Phenytoin, 24, 25t Physiologic recorder, 41 Plateau phase of action potential, 7 Posterior septal bypass tract ablation, 229–231, 230f Post-ventricular atrial refractory period (PVARP), 99 PR interval, 4, 47f, 49, 50 AV node inﬂuence, 9 prolongation, Mobitz type I block, 75 Premature beat/impulse extrastimulus pacing, 84 pacing, induction by, 39 reentrant tachycardia, 17, 18, 18f, 53, 54f Premature ventricular (PV) complexes, 160, 162 Premature ventricular contractions (PVCs), 279 Proarrhythmia, 27, 29, 30t Procainamide, 24, 25t Programmed stimulation, 39, 40f equipment, 40 reentrant arrhythmias, 39, 53–55, 54f reentrant ventricular arrhythmias, 171–176, 172t, 173f termination, 176–177 Propafenone, 25t, 26, 142 Pulmonary veins atrial ﬁbrillation trigger, 238–239 isolation, 238–239 stenosis, 239 Purkinje ﬁbers, 4, 91 action potential, 6f, 9

294

Index

Q waves, 275–276 QRS complex, 47f, 50 AV block localization, 78 AV nodal reentrant tachycardia, 128–129 bundle branch reentrant tachycardia, 248 depolarization representation, 11 duration, 49, 50 intraventricular conduction delay, 91 reentrant ventricular arrhythmias, 163, 240 ventricular dyssynchrony, 254 QT interval prolonged, 29, 190 repolarization representation, 11 triggered activity ventricular arrhythmias, 188, 189f Quadripolar electrode catheter, 37, 37f Quinidine, 24, 25t RACE trial, 153 Radiofrequency ablation, 212–214 advantages/disadvantages, 213–214 atrial ﬁbrillation in bypass tracts, 144 catheters, 213 complications, 251–252 direct current shock versus, 213–214 Recording, 35–40 Reentrant arrhythmias See also speciﬁc types antiarrhythmic drug effects, 55–56 atrial ﬂutter, 234, 234f autonomic maneuver effect, 55–56 device effects, 55–56 electrogram recording during, 55 evaluation of, 52–56 programmed stimulation, 39, 53–55, 54f Reentrant supraventricular tachycardias, 103, 106–109, 118 atrial ﬁbrillation, 108–109, 109f atrial ﬂutter, 108–109, 108f AV nodal, 106, 107f, 121–130 See also Atrioventricular (AV) nodal reentrant tachycardia bypass tract-mediated macroreentrant, 107, 107f intraatrial, 107–108, 107f, 155, 156, 156f P waves, 155, 156f SA nodal, 108, 155, 156f Reentrant tachycardia, 16–20, 17f antiarrhythmic drugs, 26–27, 28f criteria for, 16, 17f electrode catheter location, 53 initiation, 17, 18f mapping, 31 pacemaker-mediated, 98–99, 99f pacing protocols, 53, 55 supraventricular See Reentrant supraventricular tachycardias termination, 18, 19f ventricular See Reentrant ventricular tachycardia Reentrant ventricular tachycardia, 19, 160t, 161–184 See also speciﬁc types clinical characteristics, 165–170, 166f, 167f, 169t drug effect testing, 178–179, 179f “dunk tank model,” 180–181, 182f electrophysiologic study of, 170–183 inducible, 168, 170–176, 172t, 173f, 175, 175f, 176t, 180–183, 181f, 182f mapping, 240–246, 241f, 243f, 244f, 245f non-inducible, 173, 180–183 risk factors, 57, 161–165, 164f, 164t termination of, 176–178, 177f

transcatheter ablation, 240–246 treatment, 183–184 Reﬂex syncope See Vasodepressor syncope Refractory period, 7 cycle length, impact of, 52 effective See Effective refractory period (ERP) electrophysiologic evaluation, 50–52, 51f relative (RRP), 50–51, 51f AV node, 85 reentrant arrhythmias, 53 Repolarization, 7, 11 Resting phase, 7–8, 8f Retrograde conduction, reentrant tachycardia, 17 Reverse modeling, cardiac resynchronization therapy, 256–257 Right bundle branch block (RBBB), 91–92 Right free wall bypass tract ablation, 227–228, 228f Right ventricular dysplasia, 191 Romano-Ward syndrome, 190 SA See entries beginning sinoatrial (SA) Seldinger technique, modiﬁed, 42–43 Serial drug testing, 159, 178–179, 179f, 180, 194 Severity assessment, 279–283 Sick sinus syndrome, 12, 59, 60 Signal-averaged surface ECG reentrant ventricular arrhythmias, 163, 164f, 165 syncope, 269, 276 ventricular tachycardia, 269 Sinoatrial conduction time (SACT), 65–68, 65f, 69 measurement, 65–68, 66f, 67f Sinoatrial (SA) nodal reentrant supraventricular tachycardias, 108, 155, 156f Sinoatrial (SA) node, 3, 59–73 ablation, 70, 72 action potential, 9, 9f anatomy, 59 automaticity See also Sinus node recovery time (SNRT) assessment, 47–48, 61 disordered, 61 insufﬁciency, 12 autonomic innervation, 10 conduction time See Sinoatrial conduction time (SACT) dysfunction, 59–61 assessment guidelines, 69 pacemaker selection, 100–101 electrophysiologic evaluation, 61–69 indications for, 68–69 exit block, 65, 65f ﬁbrosis, 60 inappropriate sinus tachycardia See Inappropriate sinus tachycardia (IST) intrinsic heart rate, 68 normal sinus rhythm generation, 8 overdrive suppression, 47–48 reentry, electrophysiologic study in, 147–148 Sinus bradycardia, 12, 13f, 59, 60 intrinsic heart rate and, 68 pacemaker indications, 93 Sinus node dysfunction, syncope, 267–268 Sinus node recovery time (SNRT), 61–65, 69 abnormal, 62f, 64 corrected (CSNRT), 64

Index 295 measuring, 61–65 normal, 62f, 64 Sinus rhythm normal, generation, 8 restoration in atrial ﬁbrillation, 151 Sinus tachycardia, 15, 68 See also Inappropriate sinus tachycardia (IST) Sodium channels class I antiarrhythmics, 22, 23f genetic abnormalities, 192 triggered activity tachycardia, 20 Sodium ions, 7 Sotalol, 26 ST segment, 11 Strauss method, 67 Sudden Cardiac Death in Heart Failure Trial (SCD-HeFT), 200, 209 Sudden death prevention, 284, 286–287 risk, 281, 282t electrophysiologic studies and, 57 sinus node dysfunction, syncope and, 267 ventricular arrhythmias and, 158–161, 166, 167f, 185, 286 tachycardia and syncope, 270 “Sudden death survivors,” 166, 168 Sudden unexpected nocturnal death syndrome (SUNDS), 192 Supraventricular tachycardias, 31, 103–157 antegrade activation, 114–117 automatic, 104–105, 105f autonomic maneuver effect, 118 baseline recording, 111f bypass tract-mediated, 120–121, 130–146 atrial/ventricular activation patterns, 138, 139f electrophysiologic study, 133–142 P wave, 155, 156f types, 130–131, 131f classiﬁcation, 104–109 drug effects, 118–119 electrode catheter positioning, 43, 110 electrophysiologic study, 109–121 indications for, 154–157, 156f procedure, 119–121 evaluation, 110–121 initiation, 110–114 intracardiac recording of, 55 macroreentrant, 133–142 atrial preexcitation, 139, 140f, 141 atria/ventricle requirement in, 139–141, 140f initiation, 135–138, 136f, 137f mechanism of, 133–134, 134f P wave QRS complex relationship in, 141, 141f termination, 138 treatment, 141–142 pacing during, 55 reentrant See Reentrant supraventricular tachycardias reentrant circuits, 18–19 retrograde activation, 114–117, 117f, 120 syncope caused by, 268 termination, 110–114 ventricular tachycardia differentiation, 168–170, 169t Surface ECG See Electrocardiogram (ECG) Sympathetic tone automaticity effect, 9–10 conduction velocity effect, 52

reentrant supraventricular tachycardia, 118 refractory period effect, 52 Symptom relief, 285–286 treatment goal, 284 Symptom severity classiﬁcation, 283, 283t Syncope, 266–277, 282 AV block, 268 bradycardias that cause, 266–268 electrophysiologic testing, 280 etiology, 266–274, 267t evaluation, 274–277, 275t exercise-related, 276 pacemaker indications, 94 reentrant ventricular arrhythmias, 168 sinus node dysfunction, 267–268 tachycardias that cause, 268–270 vasodepressor See Vasodepressor syncope Systemic embolization, pulmonary vein isolation risk, 239 T wave, 11, 186 Tachyarrhythmias See Tachycardias Tachycardia zone, 19, 26 macroreentrant supraventricular tachycardia, 135, 141 supraventricular tachycardia initiation, 112–114 Tachycardias, 14–21 See also speciﬁc types automatic, 15–16, 16f, 20 antiarrhythmic drugs, 26 electrophysiologic study in, 48 pacemakers for, 56 pacemakers, 32 right ventricular outﬂow tract ablation, 247 sinus, 15, 68 See also Inappropriate sinus tachycardia (IST) syncope cause, 268–270 triggered activity, 20–21, 21f, 29 Therapeutic endpoints, 278, 284 Tilt table testing, 273, 276, 277 Tissue Doppler echocardiography (TDE), 263 Tocainide, 24, 25t Torsades de pointes, 21, 29, 186 Transcatheter ablation, 211–252 atrial ﬂutter, 150 AV junction, 214–216 AV nodal reentry, 130 tachycardia, 216–221, 217–219f, 221f bundle branch reentry, 192 bypass tracts, 222–233 direct current shocks, 212 intraatrial reentry, 147 macroreentrant supraventricular tachycardia, 142 mapping methods, 250–251 principles of, 211 radiofrequency energy, 212–214 right ventricular dysplasia, 191 success of, 211 supraventricular tachycardia, 157 tachycardias, 31 technology of, 211–214 ventricular tachycardia, 247–250 outﬂow tract, 191 reentrant, 170, 240–246 Transesophageal echocardiography, 151 Transmembrane potential, 5–6 depolarization phase, 6 repolarization phase, 7 resting, 5 Transmural myocardial infarction, 11 Treatment plan design, 279, 285–287

296

Index

Triggered activity tachycardias, 20–21, 21f, 29 ventricular arrhythmias See Ventricular arrhythmias, triggered activity TU wave, 186–187, 188f U wave, 186 V deﬂection, 47f, 49 V spike, 79, 80f VA conduction, normal, 115–116, 116–117f VA interval, supraventricular tachycardia, 116–117f, 120 Vagal maneuvers, 155 See also Autonomic maneuvers Vasodepressor syncope, 270–274 clinical features, 271–272 mechanism of, 271 pacemaker indications, 94 syndromes of, 270, 271t tilt table testing, 273 treatment, 273–274 Vasovagal syncope See Vasodepressor syncope Ventricles See also entries beginning ventricular electrode catheter positioning in, 44–45 myocardium of, 4 AV nodal reentrant tachycardia, 128 reentrant supraventricular tachycardias, 106 reentrant ventricular arrhythmias, 161 Ventricular arrhythmias, 158–210 See also speciﬁc types automatic, 160t, 184–185 Brugada syndrome, 192 bundle branch reentry, 192 evaluation, 160–210 idiopathic left ventricular tachycardia, 191 mechanisms of, 160–161, 161t mitral valve prolapse association, 193 outﬂow tract ventricular tachycardia, 191 right ventricular dysplasia, 191 serial drug testing, 159, 178–179, 179f, 180, 194 sudden death and, 158–161, 166, 167f, 185, 286 sudden unexpected nocturnal death syndrome, 192 treatment, 193–210 high-risk patients, 208f, 209–210

triggered activity, 160t, 185–190 catechol-dependent, 186, 187f, 190 pause-dependent, 186–190, 187f, 188f, 189f Ventricular dyssynchrony, 254, 255f, 256 See also Cardiac resynchronization therapy (CRT) measurement, 263 Ventricular ectopy antiarrhythmic drug effects, 194 complex, 283 proarrhythmic effect of antiarrhythmics, 27 treatment, 284 reentrant ventricular arrhythmias, 162, 163 Ventricular ﬁbrillation localization, 240 reentrant ventricular arrhythmias, 165–166, 167f degeneration, 177–178, 177f sudden death, 159 Ventricular pacing AV nodal reentry initiation, 125, 126f electrode catheter positioning, 43 reentrant supraventricular tachycardia, 120 Ventricular tachycardia, 21 ablation, 247–250 catecholamine-dependent, 56 electrophysiologic testing, 280 ﬁgure-of-eight model, 242, 243f, 244f idiopathic left, 191 implantable cardioverter-deﬁbrillator, 32 inducible, 168 reentrant See Reentrant ventricular tachycardia repetitive monomorphic, 191 supraventricular tachycardia differentiation, 168–170, 169t syncope caused by, 268–270 Verapamil, 144 V-V interval, 262–263 VVI pacemakers, 95–97, 96f VVIR pacemakers, 96 Wenckebach block See Mobitz type I block (Wenckebach block) Wenckebach conduction AV nodal reentry, 129 macroreentrant supraventricular tachycardia, 141 retrograde, 128 Wenckebach cycle length, 89, 125 Wolff-Parkinson-White syndrome, 131, 132f